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Review

A Proposal for a Classification Guiding the Selection of Appropriate Antibiotic Therapy for Intra-Abdominal Infections

by
Massimo Sartelli
1,*,
Francesco Cristini
2,
Federico Coccolini
3,
Francesco Maria Labricciosa
4,
Walter Siquini
1 and
Fausto Catena
5
1
Department of Surgery, Macerata Hospital, 62100 Macerata, Italy
2
Infectious Disease Department, Rimini Hospital, 47926 Rimini, Italy
3
General, Emergency and Trauma Department, Pisa University Hospital, 56126 Pisa, Italy
4
Global Alliance for Infections in Surgery, 62100 Macerata, Italy
5
General and Emergency Surgery Department, Bufalini Hospital, 47521 Cesena, Italy
*
Author to whom correspondence should be addressed.
Antibiotics 2022, 11(10), 1394; https://doi.org/10.3390/antibiotics11101394
Submission received: 14 September 2022 / Revised: 8 October 2022 / Accepted: 10 October 2022 / Published: 12 October 2022
Versions Notes

Abstract

:
Adequately controlling the source of infection and prescribing appropriately antibiotic therapy are the cornerstones of the management of patients with intra-abdominal infections (IAIs). Correctly classifying patients with IAIs is crucial to assessing the severity of their clinical condition and deciding the strategy of the treatment, including a correct empiric antibiotic therapy. Best practices in prescribing antibiotics may impact patient outcomes and the cost of treatment, as well as the risk of “opportunistic” infections such as Clostridioides difficile infection and the development and spread of antimicrobial resistance. This review aims to identify a correct classification of IAIs, guiding clinicians in the selection of the best antibiotic therapy in patients with IAIs.

1. Introduction

Intra-abdominal infections (IAIs) are an important source of patient morbidity and may be associated with poor outcomes. Treatment of patients with IAIs has been described in the literature to have satisfactory results if the management is adequate. In many studies, inclusion criteria limit the enrolment of critically ill patients, while in observational studies enrolling patients with no restrictions in inclusion criteria the mortality rate is higher. The Complicated Intra-Abdominal Infection Observational (CIAO) study, the Complicated Intra-Abdominal Infection Observational Worldwide (CIAOW) study, and the World Society of Emergency Surgery (WSES) Complicated Intra-Abdominal Infections Score Study (WISS) study showed mortality rates of 7.5%, 10.5%, and 9.2%, respectively [1,2,3].
Due to restrictive criteria, clinical trials usually over-represent patients who have perforated appendicitis, and patients enrolled in clinical trials have often a high likelihood of survival, because trial eligibility criteria usually restrict the inclusion of patients with serious comorbidities that can increase the death rate of patients [4].
Patients with IAIs should be classified correctly and stratified into low-risk and high-risk groups [5]. Many risk factors have been identified in the literature [6]. These can be related to comorbidities, patient characteristics, and physiological changes associated with the infection; to the adequacy and timing of source control; and/or to the likely presence of multidrug-resistant organisms (MDROs), leading to an ineffective initial empiric antimicrobial therapy.
Correctly classifying patients with IAIs is crucial to assessing the severity of their clinical condition and deciding the strategy of the treatment, including an appropriate empiric antibiotic therapy.
Adequate source control and appropriate antibiotic therapy are the cornerstones in the management of IAIs. There is general consensus that source control is pivotal in the management of IAIs, where both controlling the source of infection and controlling the ongoing contamination are very relevant to improving outcomes. Even if not definitively evaluated by randomised control trials, the increase in death and other adverse outcomes associated with inadequate source control demonstrates that it is of primary importance in treating patients with IAIs [7,8].
In patients with IAIs, antibiotic therapy is also important. It aims to eradicate the residual bacterial infection after source control. In addition, some uncomplicated IAIs (as in the case of some uncomplicated cases of acute appendicitis and acute cholecystitis) can now be treated only with antibiotic therapy. Best practices in prescribing antibiotics may influence patient outcomes and the cost of treatment, as well as the risk of “opportunistic” infections such as Clostridioides difficile and the spread of antibiotic resistance in the individual patient and the broader environment. There is evidence that inappropriate empiric antibiotic therapy is associated with treatment failure and poor patient outcomes [9,10,11,12].
The appropriateness of the initial empiric antibiotic therapy prescribed for IAIs is crucial, because at least 24–48 h is required to obtain standard microbiological data to target the antibiotic therapy. Core components of antibiotic prescription practices include the following: adequacy of empiric antibiotic therapy; timing of antibiotic therapy; optimisation of pharmacokinetic/pharmacodynamic (PK/PD) parameters; length of treatment; and reassessment of antibiotic therapy based on the microbiological results and susceptibility testing.
In 2016, the WSES published the executive summary of a consensus conference held on July 23, 2016, in Dublin, Ireland, covering all aspects of the management of IAIs [13]. The first recommendation states that the anatomical extent of infection, the presumed pathogens involved, any individual patient risk factors for difficult-to-treat pathogens, and the patient’s clinical condition should always be assessed independently in classifying patients with IAIs.
This review was designed to identify a correct classification of IAIs, guiding clinicians in the selection of the best antibiotic therapy for patients with IAIs.

2. Anatomical Extent of Infection

IAIs represent a heterogeneous group of infections of abdominal origin, ranging from simple acute appendicitis to more complex diffuse peritonitis. A universally accepted classification divides intra-abdominal infections into uncomplicated and complicated cases [14,15].
Uncomplicated IAIs are those infections that, originating from an abdominal organ, remain confined to the same organ, without extending to the peritoneum. In general, patients with uncomplicated IAIs can undergo only surgery or only antibiotic therapy (as in the case of the conservative treatment of uncomplicated acute appendicitis or acute cholecystitis) [16,17,18]. Moreover, in patients with uncomplicated IAIs, when source control is managed adequately, postoperative antibiotics are not necessary [16]. Uncomplicated acute left colonic diverticulitis, in which clinical observation without antibiotic therapy is generally suggested, is excluded from this classification [19].
Complicated IAIs are those infections that, originating from an abdominal organ, extend into the peritoneum, giving rise to peritonitis. Patients with complicated IAIs always require both antibiotic therapy and source control [20]. Nonetheless, there are borderline intra-abdominal conditions that are difficult to categorise as complicated or uncomplicated IAIs, such as localised colonic diverticulitis or periappendiceal phlegmon, which are complicated IAIs but may be managed with antibiotic therapy alone, without a source control procedure.
Patients with complicated IAIs are characterised as manifesting secondary peritonitis. Depending on the peritoneal extent of the infectious process, complicated IAIs are divided into localised and generalised.
Complicated IAIs are localised when the extent of the infectious process is contained by the peritoneal defence mechanisms. They are common in patients with complicated diverticulitis and appendicitis that, although evolving into perforation, can contain the infectious process through an effective peritoneal reaction and with local defence mechanisms, forming a circumscribed secondary acute peritonitis.
Complicated diffuse IAIs, on the other hand, represent the consequence of a massive contamination of the entire peritoneal cavity, following the inability of the patient’s peritoneal defence mechanisms to limit the extent of the intra-abdominal infectious process, forming a secondary acute diffuse peritonitis.
In patients with complicated IAIs, when source control is complete, a short course (3–5 days) of postoperative therapy is generally suggested. This has been confirmed by a prospective control trial (STOP-IT) published in 2015 [21]. The study randomised 260 patients with IAIs undergoing adequate source control and receiving antibiotic therapy until 2 days after the resolution of physiological abnormalities such as fever, leukocytosis, and ileus, with a maximum of 10 days (control group), and 258 receiving a fixed course of antibiotics (experimental group) for 4  ±  1 days. In patients with complicated IAIs undergoing an adequate source control procedure, the outcomes after a fixed duration of antibiotic therapy of approximately 4 days were similar to those after a longer course of antibiotics of approximately 8 days extending until after the resolution of physiological abnormalities. Among the enrolled patients, most of them were not severely ill.
Patients who have ongoing signs of infection or systemic signs of inflammation beyond 5–7 days of antibiotic treatment should warrant a diagnostic investigation to address an ongoing source of infection or failure of antibiotic therapy, and to determine whether a re-laparotomy is necessary.
The limit of this classification is that it does not really describe the complexity of the patient and can create confusion by mixing elements of the extension of the infectious process and severity of the disease expression [22]. On the other hand, in its simplicity, this classification has the advantage of classifying the extension of the infection by identifying which patients always need both antibiotic therapy and source control.
Finally, patients with complicated IAIs may be characterised as manifesting tertiary peritonitis. There is much less agreement regarding what is meant by tertiary peritonitis. It is typical of critically ill or immunocompromised patients and is often associated with multidrug-resistant organisms (MDROs). It is typically associated with poor patient outcomes and is generally considered to be a distinct form of peritonitis [23,24,25]. Tertiary peritonitis is generally described as a persistent or recurrent peritonitis occurring >48 h after apparently adequate surgical source control. It is an evolution of secondary peritonitis and should not be considered as a distinct entity. The term “ongoing peritonitis” [26] or “persistent peritonitis” [27] may better indicate the physiopathology of this clinical condition.

3. Presumed Pathogens Involved and Individual Patient Risk Factors for Difficult-to-Treat Pathogens

A classification according to the place where the patient contracts the infection divides the IAIs into community-acquired (CA-IAIs), if acquired in the community, or hospital-acquired (HA-IAIs), if acquired in a hospital or in health residences.
“Healthcare-associated infection” (HCAIs) is a commonly used term for describing infections acquired during the course of receiving healthcare, including not only hospital-acquired infections but also infections in patients living in long-term care facilities, recently hospitalised, or undergoing recent aggressive medical therapies. However, in the setting of HCAIs, there are few data regarding the concept of HCAIs as opposed to hospital-acquired infections [28].
Differentiating patients with CA-IAIs from patients with HA-IAIs allows the identification of patients with increased likelihood of IAIs caused by MDROs.
Unlike CA-IAIs, HA-IAIs show a poorer prognosis and require more aggressive antibiotic therapy. HA-IAIs usually occur after a period of hospitalisation—often after surgery, and in patients already treated with antibiotic therapy. From a microbiological point of view, CA-IAIs are characterised by the presence of bacteria usually residing in the gastrointestinal tract, and are therefore generally predictable [1,2]. HA-IAIs often involve multidrug-resistant and unpredictable bacteria, in terms of both the bacterial species involved and their sensitivity to antibiotics.
Among patients with HA-IAIs, those with postoperative peritonitis may be associated with increased mortality due to underlying patient comorbidity, atypical presentation due to non-specific clinical signs, and risk factors for acquiring MDROs and Candida spp. infections [29,30,31].
Antibiotics for empiric treatment of CA-IAIs should cover enteric Gram-negative aerobic and facultative bacteria, enteric Gram-positive streptococci, and obligate anaerobic bacilli such as Bacteroides fragilis (especially for IAIs derived from the distal small bowel, appendix, or colon) [32]. The most commonly isolated Gram-negative facultative organism is Escherichia coli [1,2].
Due to the increasing prevalence of Enterobacterales resistant to amoxicillin/clavulanate observed in community-acquired infections, caution should be taken in using amoxicillin/clavulanate in settings with a high local rate of resistance to this antibiotic.
However, most Enterobacterales remain susceptible to piperacillin/tazobactam. Its broad-spectrum activity makes it an attractive option in the management of CA-IAIs, especially in critically ill patients or in patients with CA-IAIs with other risk factors of adverse outcomes—including advanced age (70 years of age or older); presence of malignant disease; major compromise of cardiovascular, hepatic, or renal function; and hypoalbuminemia [6].
Most isolates of E. coli and other Enterobacterales in CA-IAIs remain susceptible to third-generation cephalosporins. Among third-generation cephalosporins, cefotaxime or ceftriaxone in association with metronidazole may be options for empiric therapy of CA-IAIs in patients with no risk factors for ESBLs. Cefepime is a fourth-generation cephalosporin, with broader-spectrum activity than ceftriaxone. It is poorly hydrolysed by AmpC beta-lactamase, allowing it to be effective against AmpC-producing organisms [15]. For empiric therapy, cefepime must be combined with metronidazole, because it is inactive against anaerobes.
In recent years, fluoroquinolones have been widely used in the treatment of IAIs due to their activity against aerobic Gram-negative bacteria and tissue penetration. The worldwide increase in resistance among E. coli and other Enterobacterales has limited the use of fluoroquinolones for empiric treatment of CA-IAIs, and they are generally suggested in association with metronidazole and only in non-critically ill patients with allergy to beta-lactam agents.
In the context of complicated IAIs, the main resistance burden is posed by ESBL-producing Enterobacterales, which are prevalent in hospital-acquired infections but are also observed in community-acquired infections [33,34]. ESBLs are enzymes able to hydrolyse and inactivate a wide variety of beta-lactams, such as third-generation cephalosporins, penicillins, and aztreonam [35,36]. Most ESBLs of clinical interest are encoded by genes located on plasmids. They are able to carry genes encoding resistance to other classes of antibiotics, including aminoglycosides and fluoroquinolones [36]. Although routine testing for ESBLs is not performed by most microbiology laboratories [37], non-susceptibility to ceftriaxone (MICs ≥ 2 mcg/mL) may be used to confirm ESBL infections. However, recognising ESBLs on the basis of susceptibility to ceftriaxone may present limitations, as bacteria that are not susceptible to ceftriaxone due to mechanisms other than ESBL production may be incorrectly presumed to be ESBL-producers [38,39].
ESBLs generally should not be covered in patients with CA-IAIs with no signs of severity or without risk of treatment failure, except in regions with particular local epidemiological conditions, where there is a high likelihood that ESBL-producing Enterobacterales may be components of the infection.
Risk factors of ESBL-producing Enterobacterales in CA-IAIs include recent exposure to antibiotics (particularly third-generation cephalosporins or fluoroquinolones) and known colonisation with ESBL producing Enterobacterales. These aspects should always be considered in stratifying patients with CA-IAIs to prescribe an adequate empiric therapy.
Carbapenems have been considered the empiric antibiotics of choice for treating patients with ESBL-producing Enterobacterales. Group 1 carbapenems include ertapenem—a once-a-day carbapenem sharing the same activity of Group 2 carbapenems against ESBL-producing Enterobacterales. However, it is not active against Pseudomonas aeruginosa and enterococci [40]. Group 2 includes imipenem/cilastatin, meropenem, and doripenem. Compared to ertapenem, they have activity against non-fermentative Gram-negative bacilli. Unlike meropenem and doripenem, imipenem/cilastatin is active against enterococci that are susceptible to ampicillin.
However, in order to avoid excessive carbapenem use, carbapenem-sparing strategies using other antibiotics—such as piperacillin/tazobactam, an aminoglycoside agent, tigecycline, or eravacycline—should be considered.
The significance of piperacillin/tazobactam for treating ESBL-producing Enterobacterales has been a debated issue. Gram-negative bacteria have the ability to concomitantly produce multiple ESBLs as well as AmpC beta-lactamases and can possess other mechanisms of resistance limiting the activity of piperacillin/tazobactam [41]. On the other hand, the activity of piperacillin/tazobactam is influenced by the “inoculum effect”—a laboratory phenomenon described as a significant increase in the MIC of an antibiotic when a great number of bacteria are inoculated [41].
An RCT conducted in patients with ESBL-producing Enterobacterales bloodstream infections [42] demonstrated inferior results of piperacillin/tazobactam compared to carbapenems. Although piperacillin/tazobactam is not considered the first-choice antibiotic to treat ESBL-producing Enterobacterales [43], it may still be considered a valuable carbapenem-sparing agent in the management of ESBLs in IAIs treated with adequate source control when dealing with fully susceptible bacteria (MIC ≤ 8 mg/L). A high dose (18 g) should be prescribed to optimise PK/PD targeting in critically ill patients [44].
Aminoglycosides have in vitro activity against aerobic Gram-negative bacteria, including ESBL-producing Enterobacterales, and act synergistically against certain Gram-positive bacteria.
Because of their serious toxic side effects, including nephrotoxicity and ototoxicity, some authors do not recommend aminoglycosides for the routine empiric treatment of IAIs [6]. They may be reserved for patients with allergies to beta-lactam agents or used in combination with beta-lactam agents [45]. In any case, this class of antibiotics remains an important option to treat Gram-negative bacteria and widen the spectrum of antibiotic therapy when resistant organisms are suspected.
Tigecycline remains a useful option for treating patients with complicated IAIs, due to its favourable activity against anaerobic organisms, enterococci, and ESBLs [46]. It has no in vitro activity against P. aeruginosa or certain Enterobacterales, including Proteus spp. and Serratia spp. Excess mortality was observed in patients treated with tigecycline when compared with other antibiotics [47]. Study-level and patient-level analyses demonstrated that, in particular, patients with ventilator-associated pneumonia and baseline bacteraemia were at a higher risk of mortality. A mortality analysis was used to investigate the association of baseline factors with clinical failure and mortality in complicated IAIs and did not suggest that tigecycline was a factor either for failure or for death in phase 3 and 4 comparative clinical trials of tigecycline [48]. Tigecycline should not be considered the first-line option for treating hospital-acquired pneumonia and bacteraemia.
Eravacycline is an antibiotic that is structurally similar to tigecycline. Eravacycline demonstrates broad-spectrum activity against Gram-positive, Gram-negative—including ESBLs-producing Enterobacterales—and anaerobic bacteria. Like tigecycline, it is inactive against P. aeruginosa [49]. Eravacycline is well-tolerated with nausea and vomiting and, interestingly, is also available for oral administration.
Finally, ceftolozane/tazobactam and ceftazidime/avibactam have shown efficacy in treating patients with IAIs caused by ESBL-producing Enterobacterales [50,51]. They may be especially useful in critically ill patients when dealing with isolates exhibiting high MIC values [44]. In settings with a high prevalence of carbapenem-resistant Enterobacterales (CRE), ceftazidime/avibactam should be reserved for the treatment of CRE.
Among Gram-negative bacteria, carbapenem-resistant Enterobacterales represent a heterogeneous group of bacteria with more potential mechanisms of antibiotic resistance. They are generally divided into carbapenemase-producing Enterobacterales and non-carbapenemase-producing Enterobacterales. Carbapenemases hydrolyse penicillins, all cephalosporins, beta-lactamase inhibitors, and even carbapenems. The most widespread carbapenemases are Klebsiella pneumoniae carbapenemases [52,53,54,55]. These are rapidly emerging as an important source of hospital-acquired infections in many regions of the world. Metallo-beta-lactamases (MBLs) differ from the other beta-lactamases in their requirement of zinc for activity. MBLs are all capable of hydrolysing most beta-lactam agents, including carbapenems, except for the monobactam aztreonam.
Alarming rates of resistance to many antibiotics in health facilities worldwide have been reported for non-fermenting Gram-negative bacteria, including P. aeruginosa, Stenotrophomonas maltophilia, and Acinetobacter baumannii. Non-fermenting Gram-negative bacteria are intrinsically resistant to many antibiotics; moreover, they can acquire additional resistance to other important antibiotic agents. These mechanisms may be present simultaneously and can confer resistance to different classes of antibiotics.
Various mechanisms of resistance have been identified in P. aeruginosa, including membrane permeability defects, expression of efflux pumps, and production of antibiotic-hydrolysing enzymes such as AmpC beta-lactamases or carbapenemases. The most prevalent carbapenemases in P. aeruginosa are MBLs, such as Verona integron-encoded metallo-β-lactamase (VIM) and imipenemase (IMP) types.
In recent years, several new antibiotics with predominant activity against Gram-negative bacteria have been approved by the U.S. Food and Drug Administration (FDA) and the European Medicines Agency (EMA). Meropenem/vaborbactam, ceftazidime/avibactam, and imipenem/cilastatin/relebactam are the options for carbapenemase-producing K. pneumoniae infections [56,57,58,59,60,61,62,63,64,65].
The lack of in vitro activity of ceftazidime/avibactam against metallo-beta-lactamase (MBL) and the observation that many MBL-producing infections can coproduce other beta-lactamases—including ESBLs, AmpC, and OXA-48—suggest a potential effect of combining ceftazidime/avibactam with aztreonam, which is not hydrolysed by MBLs [66,67,68].
Ceftazidime/avibactam is the preferred treatment option for OXA-48-like-producing Enterobacterales. It has no activity against anaerobic bacteria.
Ceftazidime/avibactam in combination with aztreonam or cefiderocol [66] as monotherapy are the preferred treatment option for MBL-producing Enterobacterales.
Due to its epithelial lining fluid penetration, meropenem-vaborbactam should be used as first therapeutic choice in patients with ventilator-associated pneumonia due to KPC-producing Enterobacterales.
Cefiderocol appears to be effective in vitro against all resistance phenotypes of P. aeruginosa, including MBLs. Cefiderocol is also effective in vitro against extreme drug resistant A. baumannii. Despite these promising early data, a recent clinical trial did not support the higher effectiveness of cefiderocol in the patient subset with A. baumannii infections [69]. Therefore, further clinical data are needed to better understand the role of this novel option [70].
Local epidemiological data for selecting an adequate empiric antibiotic therapy in patients with HA-IAIs at risk of infection with drug-resistant Gram-negative bacteria can be useful to define the appropriate antibiotic approach.
Among Gram-positive bacteria, the pathogenicity of enterococci in IAIs has been a debated issue [71,72,73,74], also hypothesising a synergistic effect with other bacteria such as E. coli and anaerobes [75,76,77]. Some studies have demonstrated poor outcomes in patients with HA-IAIs, especially in critically ill patients [72,73]. In this setting, coverage against enterococci should be always considered. Although Enterococcus isolation was not found to be an independent risk factor for the composite outcomes in non-critically ill patients in a post hoc analysis of the STOP-IT trial database [74], patients who had previously received cephalosporins or other antibiotics for enterococci, immunocompromised patients, and patients with valvular heart disease or prosthetic intravascular materials were also considered to need coverage against enterococci [32].
Most strains of Enterococcus faecalis are susceptible to ampicillin. In patients with IAIs, Enterococcus faecium is increasingly encountered—particularly in patients with HA-IAIs. In contrast to E. faecalis, nearly all strains of E. faecium are resistant to ampicillin [78,79]. First-line treatment of vancomycin-susceptible strains of E. faecium includes vancomycin or other glycopeptides, such as teicoplanin. The incidence of vancomycin-resistant E. faecium (VRE) is increasing. The acquisition of glycopeptide resistance by enterococci can seriously affect the treatment and control of these organisms in patients with hospital-acquired infections [71]. Linezolid and daptomycin may be used for the management of suspected or proven infections caused by VRE.
Staphylococcus aureus is not common in patients with IAIs. It is rarely isolated in patients with CA-IAIs, but it may be found to some extent in patients with HA-IAIs and may be resistant to methicillin (MRSA). Patients with HA-IAIs, those colonised with MRSA, and those with multiple healthcare-associated risk factors for MRSA colonisation—including previous hospitalisation or surgery—and significant recent exposure to antibiotics may be considered at risk of infection by MRSA. Glycopeptides such as vancomycin may be used for the treatment of IAIs to provide therapy for suspected or proven infections caused by vancomycin-susceptible MRSA. S. aureus strains with increased resistance to vancomycin—known as vancomycin-intermediate-resistant S. aureus (VISA), exhibiting an MIC of 4–8 µg/mL, and S. aureus completely resistant to vancomycin (VRSA), exhibiting an MIC ≥ 16 µg/mL—are increasing [80]. Linezolid and daptomycin may be used for the management of suspected or proven infections caused by VRSA.

4. Patients’ Clinical Condition

Grading of the clinical severity of patients with IAIs has been well described by the sepsis definitions [81]. A prospective observational study involving 180 consecutive patients with secondary generalised peritonitis (community-acquired and postoperative) showed that patients with septic shock had a higher mortality rate than patients without shock (35% versus 8%).
The data from the WISS study [3] showed that mortality was significantly affected by sepsis and that mortality rates increased in patients developing organ dysfunction and septic shock. Sepsis-related mortality was as follows: no sepsis = 1.2%, sepsis only = 4.4%, severe sepsis = 27.8%, and septic shock = 67.8%.
In February 2016, a proposal for new definitions for sepsis (Sepsis-3) was published in the Journal of the American Medical Association (JAMA) [82]. These definitions updated the previous sepsis definitions [83,84]. The new definitions were intended to provide a standardised classification facilitating clinical care, reporting, and research. The Sepsis-3 definitions classify sepsis as life-threatening organ dysfunction caused by a dysregulated response of the host to infection, emphasising the potential lethality and the need for urgent recognition. Organ dysfunction is determined by an increase in the Sequential Organ Failure Assessment (SOFA) score of 2 points or more that is associated with a risk of in-hospital mortality greater than 10%. Septic shock is defined as a subset of sepsis and is clinically characterised by the requirement of vasopressor agents to maintain a mean arterial pressure of 65 mmHg or more and a serum lactate level above 2 mmol/L (>18 mg/dL) in the absence of hypovolemia.
Human immune responses to an infectious focus can vary greatly from individual to individual. Some individuals greatly overreact to infection, producing a massive cytokine storm leading to multi-organ failure. On the other hand, some individuals have little response to the same infection. Identifying patients overreacting to the infection as soon as possible and correcting the underlying dysfunction may improve patient outcomes [85,86]. An insufficient or otherwise inadequate antibiotic regimen is one of the variables more strongly associated with unfavourable outcomes in critically ill patients [87].
These findings have been confirmed in a recent meta-analysis demonstrating reduced mortality and significantly shorter hospital lengths of stay, with corresponding reductions in hospital costs, in patients receiving early appropriate versus inappropriate antibiotic therapy for severe bacterial infection [88].
The reduction in mortality associated with early administration of antibiotics is strongest in patients with septic shock. Studies have reported a strong association between time to antibiotics and mortality in patients with septic shock, but a weaker association in patients with sepsis but without septic shock.
A recent review suggests that a reasonable timeframe would be no later than 3–5 h after the onset of infection, but immediately for patients with septic shock [89]. Based on the best available data, there is a strong relationship between timing of antibiotic administration and mortality in patients with septic shock, but a less pronounced relationship in patients with sepsis and without shock [90].
The 2021 Surviving Sepsis Campaign guidelines recommend the immediate administration of antibiotics in patients with possible septic shock or a high likelihood of sepsis—ideally within 1 h from the time when sepsis was first recognised. In patients with possible sepsis without shock, the guidelines suggest a time-limited course of rapid investigation and administering antibiotics within 3 h of recognition [91].
Considering the spread of MDROs in many regions of the world and the association between delaying appropriate antibiotic therapy and worse outcomes in patients with sepsis and septic shock, the initial administration of a broad-spectrum regimen including at least one effective agent active against the suspected or proven offending organism is crucial.
Antibiotic de-escalation is now considered a key point of antimicrobial stewardship programs in intensive care units (ICUs) [92]. However, its real efficacy has been debated and has not been convincingly demonstrated in a clinical setting [93]. Even if it appears beneficial, it may have some side effects, including its use as a justification of unrestricted broad-spectrum empiric antibiotic therapy and the exposure of patients to multiple, sequential antibiotics with unwanted effects on the microbiome.
Montravers et al. [94] evaluated the characteristics and outcomes of antimicrobial de-escalation in patients with HA-IAIs, demonstrating that de-escalation is a feasible option in these patients, even if multidrug-resistant non-fermenting Gram-negative organisms may limit its implementation in the setting of IAIs. When treating patients with sepsis of abdominal origin, clinicians should be aware that antibiotic pharmacokinetics may be modified by the pathophysiology of sepsis, and should always consider the pathophysiological and immunological status of the patient [94]. In fact, antibiotics are subject to changes in PK/PD parameters in patients with sepsis and septic shock, where low antibiotic levels may be too low, risking clinical failure, or too high, risking toxicity.
The “dilution effect” should be considered for hydrophilic antibiotics—including beta-lactam agents, aminoglycosides, and glycopeptides—that selectively distribute to the extracellular space [95]. Low plasma antibiotic concentrations can contribute to lower levels in peritoneal fluid, with potentially reduced antibiotic activity in the target tissues.
Higher than standard loading doses of beta-lactam agents, aminoglycosides, fosfomycin, or glycopeptides should be administered to ensure optimal antibiotic concentration at the infection site in patients with sepsis or septic shock.
Once appropriate initial loading is administered, it is crucial to reassess the antibiotic regimen daily, because pathophysiological changes may occur, significantly affecting antibiotic distribution in critically ill patients. Lower dosages of renally excreted antibiotics should be administered in patients with impaired renal function, while higher dosages of renally excreted antibiotics are needed for optimal exposure in patients with glomerular hyperfiltration. In critically ill patients, plasma creatinine is an unreliable marker of renal function [95].
Adequate dosing is associated with the concept of time-dependent versus concentration-dependent killing. Beta-lactam agents have time-dependent activity, exerting optimal activity when antibiotic concentrations are maintained above the minimum inhibitory concentration (MIC) [95]. For beta-lactam agents, prolonged or continuous infusions have been advocated in order to maximise the time for which the drug concentration exceeds the MIC. However, a randomised controlled trial comparing continuous versus intermittent infusion of piperacillin/tazobactam in the specific setting of complicated IAIs [96] did not show different outcomes.
These results should not be generalisable to critically ill patients and patients with infections caused by less susceptible bacteria with high MIC values, where prolonged infusion with a beta-lactam agent seems to have more advantages than in patients with infections caused by sensitive bacteria [97,98].
Although there is insufficient evidence to reach definitive strong conclusions, two meta-analyses have demonstrated reduced short-term mortality with prolonged infusion of beta-lactam agents in critically ill patients [99,100]. No trials have assessed the undesirable effects of continuous infusion. However, meta-analyses evaluating the effects of prolonged infusion in subgroups of stratified patients are needed to identify the subgroup of patients benefiting most from prolonged infusion [101].
Interestingly, a recent meta-analysis evaluating prolonged versus intermittent beta-lactam antibiotics in patients with sepsis or septic shock [102] showed favourable effects of prolonged infusion in studies published in 2015 or after.
On the other hand, antibiotics such as aminoglycosides have concentration-dependent activity and should be administered in a once-daily manner (or with the least possible number of daily administrations) in order to achieve high peak plasma concentrations [95]. Nephrotoxicity related to aminoglycosides is caused by direct damage to the renal cortex and its uptake saturation. Thus, a correct dosing strategy may reduce the renal cortex’s exposure to aminoglycosides, reducing the risk of nephrotoxicity [103].
Another group of patients at high risk of treatment failure are immunocompromised patients. Immunosuppressive status includes congenital conditions such as T- or B-cell defects and macrophage dysfunctions, as well as acquired conditions such as infections with human immunodeficiency virus (HIV) developing acquired immunodeficiency syndrome, haematological malignancies or solid malignancies needing chemotherapy, and solid organ transplantation patients or those with inflammatory disease/rheumatologic disease needing immunomodulatory agents [104]. The management of these patients with IAIs should be individualised and needs an appropriate stratification to plan the most appropriate therapeutic pathways [105].

5. Conclusions

The anatomical extent of the infection, the presumed pathogens involved, the risk factors for major resistance patterns, and the patient’s clinical condition should be assessed independently so as to classify patients. This allows the stratification of patients with IAIs, guiding physicians in providing the appropriate antibiotic strategy.
To assess the anatomical extent of the infection, physicians should always determine whether the IAI is complicated or uncomplicated. Unlike patients with complicated IAIs, who always require both antibiotic therapy and source control, patients with uncomplicated IAIs do not require postoperative antibiotics when source control is managed adequately.
To assess the presumed pathogens involved and any risk factors for major resistance patterns, physicians should always determine whether the IAI is community-acquired or hospital-acquired. HA-IAIs often involve multidrug-resistant and unpredictable bacteria, in terms of both the bacterial species involved and their sensitivity to antibiotics. Among patients with HA-IAIs, those with postoperative peritonitis may be associated with increased mortality due to underlying patient comorbidity, atypical presentation due to non-specific clinical signs, and risk factors for acquiring MDROs and Candida spp. infections.
In order to assess the grading of the clinical severity of patients, physicians should always determine the patients’ sepsis condition. Identifying patients overreacting to the infection as soon as possible and administering antibiotics may improve patient outcomes, especially in patients with septic shock. The 2021 Surviving Sepsis Campaign guidelines recommend the immediate administration of antibiotics in patients with possible septic shock or a high likelihood of sepsis—ideally within 1 h from the time when sepsis was first recognised. In patients with possible sepsis without shock, the guidelines suggest a time-limited course of rapid investigation and administering antibiotics within 3 h of recognition [91].
In Table 1, Table 2, Table 3, Table 4, Table 5, Table 6, Table 7 and Table 8, proposals for antibiotic regimens for the treatment of IAIs are illustrated.
Abdominal tuberculosis (TB) is an increasingly common disease posing diagnostic challenges because of the non-specific features of the disease. Abdominal TB is a type of extrapulmonary tuberculosis that involves the abdominal organs, such as the intestines, peritoneum, and abdominal lymph nodes. It can occur either in isolation or along with a primary focus (such as the lungs) in patients with disseminated tuberculosis. This review does not refer to abdominal TB, which will be considered individually in an upcoming review.

Author Contributions

Conceptualisation and methodology, M.S.; writing and original draft preparation, M.S.; review, M.S., F.C. (Francesco Cristini), F.C. (Federico Coccolini), F.M.L., W.S. and F.C. (Fausto Catena); editing, F.M.L. All authors have read and agreed to the published version of the manuscript.

Funding

This research received no external funding.

Conflicts of Interest

The authors declare no conflict of interest.

References

  1. Sartelli, M.; Catena, F.; Ansaloni, L.; Leppaniemi, A.; Taviloglu, K.; van Goor, H.; Viale, P.; Lazzareschi, D.V.; Coccolini, F.; Corbella, D.; et al. Complicated intra-abdominal infections in Europe: A comprehensive review of the CIAO study. World J. Emerg. Surg. 2012, 7, 36. [Google Scholar] [CrossRef] [Green Version]
  2. Sartelli, M.; Catena, F.; Ansaloni, L.; Coccolini, F.; Corbella, D.; Moore, E.E.; Malangoni, M.; Velmahos, G.; Coimbra, R.; Koike, K.; et al. Complicated intra-abdominal infections worldwide: The definitive data of the CIAOW Study. World J. Emerg. Surg. 2014, 9, 37. [Google Scholar] [CrossRef] [Green Version]
  3. Sartelli, M.; Abu-Zidan, F.M.; Catena, F.; Griffiths, E.A.; Di Saverio, S.; Coimbra, R.; Ordoñez, C.A.; Leppaniemi, A.; Fraga, G.P.; Coccolini, F.; et al. Global validation of the WSES Sepsis Severity Score for patients with complicated intra-abdominal infections: A prospective multicentre study (WISS Study). World J. Emerg. Surg. 2015, 10, 61. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  4. Merlino, J.I.; Malangoni, M.A.; Smith, C.M.; Lange, R.L. Prospective randomized trials affect the outcomes of intraabdominal infection. Ann. Surg. 2001, 233, 859–866. [Google Scholar] [CrossRef] [PubMed]
  5. Swenson, B.R.; Metzger, R.; Hedrick, T.L.; McElearney, S.T.; Evans, H.L.; Smith, R.L.; Chong, T.W.; Popovsky, K.A.; Pruett, T.L.; Sawyer, R.G. Choosing antibiotics for intra-abdominal infections: What do we mean by “high risk”? Surg. Infect. 2009, 10, 29–39. [Google Scholar] [CrossRef] [PubMed]
  6. Mazuski, J.E.; Tessier, J.M.; May, A.K.; Sawyer, R.G.; Nadler, E.P.; Rosengart, M.R.; Chang, P.K.; O’Neill, P.J.; Mollen, K.P.; Huston, J.M.; et al. The Surgical Infection Society Revised Guidelines on the Management of Intra-Abdominal Infection. Surg. Infect. 2017, 18, 1–76. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  7. Martínez, M.L.; Ferrer, R.; Torrents, E.; Guillamat-Prats, R.; Gomà, G.; Suárez, D.; Álvarez-Rocha, L.; Pozo Laderas, J.C.; Martín-Loeches, I.; Levy, M.M.; et al. Impact of Source Control in Patients With Severe Sepsis and Septic Shock. Crit. Care Med. 2017, 45, 11–19. [Google Scholar] [CrossRef] [PubMed]
  8. Tellor, B.; Skrupky, L.P.; Symons, W.; High, E.; Micek, S.T.; Mazuski, J.E. Inadequate Source Control and Inappropriate Antibiotics are Key Determinants of Mortality in Patients with Intra-Abdominal Sepsis and Associated Bacteremia. Surg. Infect. 2015, 16, 785–793. [Google Scholar] [CrossRef]
  9. Guilbart, M.; Zogheib, E.; Ntouba, A.; Rebibo, L.; Régimbeau, J.M.; Mahjoub, Y.; Dupont, H. Compliance with an empirical antimicrobial protocol improves the outcome of complicated intra-abdominal infections: A prospective observational study. Br. J. Anaesth. 2016, 117, 66–72. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  10. Krobot, K.; Yin, D.; Zhang, Q.; Sen, S.; Altendorf-Hofmann, A.; Scheele, J.; Sendt, W. Effect of inappropriate initial empiric antibiotic therapy on outcome of patients with community-acquired intra-abdominal infections requiring surgery. Eur. J. Clin. Microbiol. Infect. Dis. 2004, 23, 682–687. [Google Scholar] [CrossRef]
  11. Davey, P.G.; Marwick, C. Appropriate vs. inappropriate antimicrobial therapy. Clin. Microbiol. Infect. 2008, 14 (Suppl. S3), 15–21. [Google Scholar] [CrossRef] [Green Version]
  12. Sturkenboom, M.C.; Goettsch, W.G.; Picelli, G.; in ‘t Veld, B.; Yin, D.D.; de Jong, R.B.; Go, P.M.; Herings, R.M. Inappropriate initial treatment of secondary intra-abdominal infections leads to increased risk of clinical failure and costs. Br. J. Clin. Pharmacol. 2005, 60, 438–443. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  13. Sartelli, M.; Catena, F.; Abu-Zidan, F.M.; Ansaloni, L.; Biffl, W.L.; Boermeester, M.A.; Ceresoli, M.; Chiara, O.; Coccolini, F.; De Waele, J.J.; et al. Management of intra-abdominal infections: Recommendations by the WSES 2016 consensus conference. World J. Emerg. Surg. 2017, 12, 22. [Google Scholar] [CrossRef] [Green Version]
  14. Sartelli, M. A focus on intra-abdominal infections. World J. Emerg. Surg. 2010, 5, 9. [Google Scholar] [CrossRef]
  15. Sartelli, M.; Weber, D.G.; Ruppé, E.; Bassetti, M.; Wright, B.J.; Ansaloni, L.; Catena, F.; Coccolini, F.; Abu-Zidan, F.M.; Coimbra, R.; et al. Erratum to: Antimicrobials: A global alliance for optimizing their rational use in intra-abdominal infections (AGORA). World J. Emerg. Surg. 2017, 12, 35. [Google Scholar] [CrossRef]
  16. Sartelli, M.; Coccolini, F.; Kluger, Y.; Agastra, E.; Abu-Zidan, F.M.; Abbas, A.E.S.; Ansaloni, L.; Adesunkanmi, A.K.; Atanasov, B.; Augustin, G.; et al. WSES/GAIS/SIS-E/WSIS/AAST global clinical pathways for patients with intra-abdominal infections. World J. Emerg. Surg. 2021, 16, 49. [Google Scholar] [CrossRef]
  17. Di Saverio, S.; Podda, M.; De Simone, B.; Ceresoli, M.; Augustin, G.; Gori, A.; Boermeester, M.; Sartelli, M.; Coccolini, F.; Tarasconi, A.; et al. Diagnosis and treatment of acute appendicitis: 2020 update of the WSES Jerusalem guidelines. World J. Emerg. Surg. 2020, 15, 27. [Google Scholar] [CrossRef]
  18. Pisano, M.; Allievi, N.; Gurusamy, K.; Borzellino, G.; Cimbanassi, S.; Boerna, D.; Coccolini, F.; Tufo, A.; Di Martino, M.; Leung, J.; et al. 2020 World Society of Emergency Surgery updated guidelines for the diagnosis and treatment of acute calculus cholecystitis. World J. Emerg. Surg. 2020, 15, 61. [Google Scholar] [CrossRef]
  19. Sartelli, M.; Weber, D.G.; Kluger, Y.; Ansaloni, L.; Coccolini, F.; Abu-Zidan, F.; Augustin, G.; Ben-Ishay, O.; Biffl, W.L.; Bouliaris, K.; et al. 2020 update of the WSES guidelines for the management of acute colonic diverticulitis in the emergency setting. World J. Emerg. Surg. 2020, 15, 32. [Google Scholar] [CrossRef]
  20. Sartelli, M.; Chichom-Mefire, A.; Labricciosa, F.M.; Hardcastle, T.; Abu-Zidan, F.M.; Adesunkanmi, A.K.; Ansaloni, L.; Bala, M.; Balogh, Z.J.; Beltrán, M.A.; et al. The management of intra-abdominal infections from a global perspective: 2017 WSES guidelines for management of intra-abdominal infections. World J. Emerg. Surg. 2017, 12, 29. [Google Scholar] [CrossRef] [PubMed]
  21. Sawyer, R.G.; Claridge, J.A.; Nathens, A.B.; Rotstein, O.D.; Duane, T.M.; Evans, H.L.; Cook, C.H.; O’Neill, P.J.; Mazuski, J.E.; Askari, R.; et al. Trial of short-course antimicrobial therapy for intraabdominal infection. N. Engl. J. Med. 2015, 372, 1996–2005. [Google Scholar] [CrossRef] [Green Version]
  22. Blot, S.; De Waele, J.J.; Vogelaers, D. Essentials for selecting antimicrobial therapy for intra-abdominal infections. Drugs 2012, 72, e17–e32. [Google Scholar] [CrossRef] [PubMed]
  23. Gupta, S.; Kaushik, R. Peritonitis—The Eastern experience. World J. Emerg. Surg. 2006, 1, 13. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  24. Mishra, S.P.; Tiwary, S.K.; Mishra, M.; Gupta, S.K. An introduction of tertiary peritonitis. J. Emerg. Trauma Shock 2014, 7, 121–123. [Google Scholar]
  25. Reemst, P.H.; van Goor, H.; Goris, R.J. SIRS, MODS and tertiary peritonitis. Eur. J. Surg. Suppl. 1996, 576, 47–48. [Google Scholar]
  26. Lamme, B.; Mahler, C.W.; van Ruler, O.; Gouma, D.J.; Reitsma, J.B.; Boermeester, M.A. Clinical predictors of ongoing infection in secondary peritonitis: Systematic review. World J. Surg. 2006, 30, 2170–2181. [Google Scholar] [CrossRef] [PubMed]
  27. Montravers, P.; Dufour, G.; Guglielminotti, J.; Desmard, M.; Muller, C.; Houissa, H.; Allou, N.; Marmuse, J.P.; Augustin, P. Dynamic changes of microbial flora and therapeutic consequences in persistent peritonitis. Crit. Care 2015, 19, 70. [Google Scholar] [CrossRef] [Green Version]
  28. Cardoso, T.; Almeida, M.; Friedman, N.D.; Aragão, I.; Costa-Pereira, A.; Sarmento, E.; Azevedo, L. Classification of healthcare-associated infection: A systematic review 10 years after the first proposal. BMC Med. 2014, 12, 40. [Google Scholar] [CrossRef] [Green Version]
  29. Seguin, P.; Fédun, Y.; Laviolle, B.; Nesseler, N.; Donnio, P.Y.; Mallédant, Y. Risk factors for multidrug-resistant bacteria in patients with post-operative peritonitis requiring intensive care. J. Antimicrob. Chemother. 2010, 65, 342–346. [Google Scholar] [CrossRef] [Green Version]
  30. Augustin, P.; Kermarrec, N.; Muller-Serieys, C.; Lasocki, S.; Chosidow, D.; Marmuse, J.P.; Valin, N.; Desmonts, J.M.; Montravers, P. Risk factors for multi drug resistant bacteria and optimization of empirical antibiotic therapy in postoperative peritonitis. Crit. Care 2010, 14, R20. [Google Scholar] [CrossRef] [Green Version]
  31. Lee, D.S.; Ryu, J.A.; Chung, C.R.; Yang, J.; Jeon, K.; Suh, G.Y.; Lee, W.Y.; Park, C.M. Risk factors for acquisition of multidrug-resistant bacteria in patients with anastomotic leakage after colorectal cancer surgery. Int. J. Colorectal. Dis. 2015, 30, 497–504. [Google Scholar] [CrossRef]
  32. Solomkin, J.S.; Mazuski, J.E.; Bradley, J.S.; Rodvold, K.A.; Goldstein, E.J.; Baron, E.J.; O’Neill, P.J.; Chow, A.W.; Dellinger, E.P.; Eachempati, S.R.; et al. Diagnosis and management of complicated intra-abdominal infection in adults and children: Guidelines by the Surgical Infection Society and the Infectious Diseases Society of America. Clin. Infect. Dis. 2010, 50, 133–164. [Google Scholar] [CrossRef] [PubMed]
  33. Morrissey, I.; Hackel, M.; Badal, R.; Bouchillon, S.; Hawser, S.; Biedenbach, D. A review of ten years of the study for monitoring antimicrobial resistance trends (SMART) from 2002 to 2011. Pharmaceuticals 2013, 6, 1335–1346. [Google Scholar] [CrossRef] [Green Version]
  34. Hawser, S.P.; Bouchillon, S.K.; Hoban, D.J.; Badal, R.E.; Cantón, R.; Baquero, F. Incidence and antimicrobial susceptibility of Escherichia coli and Klebsiella pneumoniae with extended-spectrum beta-lactamases in community- and hospital-associated intra-abdominal infections in Europe: Results of the 2008 Study for Monitoring Antimicrobial Resistance Trends (SMART). Antimicrob. Agents Chemother. 2010, 54, 3043–3046. [Google Scholar]
  35. Schultsz, C.; Geerlings, S. Plasmid-mediated resistance in Enterobacterales: Changing landscape and implications for therapy. Drugs 2012, 72, 1–16. [Google Scholar] [CrossRef]
  36. Perez, F.; Bonomo, R.A. Can we really use beta-lactam/beta-lactam inhibitor combinations for the treatment of infections caused by extended-spectrum beta-lactamase-producing bacteria? Clin. Infect. Dis. 2012, 54, 175–177. [Google Scholar] [CrossRef] [Green Version]
  37. Robberts, F.J.; Kohner, P.C.; Patel, R. Unreliable extended-spectrum beta-lactamase detection in the presence of plasmid-mediated AmpC in Escherichia coli clinical isolates. J. Clin. Microbiol. 2009, 47, 358–361. [Google Scholar] [CrossRef] [Green Version]
  38. Tamma, P.D.; Humphries, R.M. PRO: Testing for ESBL production is necessary for ceftriaxone-non-susceptible Enterobacterales: Perfect should not be the enemy of progress. JAC Antimicrob. Resist. 2021, 3, dlab019. [Google Scholar] [CrossRef]
  39. Mathers, A.J.; Lewis, J.S., 2nd. CON: Testing for ESBL production is unnecessary for ceftriaxone-resistant Enterobacterales. JAC Antimicrob. Resist. 2021, 3, dlab020. [Google Scholar] [CrossRef]
  40. Hammond, M.L. Ertapenem: A group 1 carbapenem with distinct antibacterial and pharmacological properties. J. Antimicrob. Chemother. 2004, 53, ii7–ii9. [Google Scholar] [CrossRef] [Green Version]
  41. Karaiskos, I.; Giamarellou, H. Carbapenem-Sparing Strategies for ESBL Producers: When and How. Antibiotics 2020, 9, 61. [Google Scholar] [CrossRef] [Green Version]
  42. Harris, P.N.A.; Tambyah, P.A.; Lye, D.C.; Mo, Y.; Lee, T.H.; Yilmaz, M.; Alenazi, T.H.; Arabi, Y.; Falcone, M.; Bassetti, M.; et al. Effect of Piperacillin-tazobactam vs meropenem on 30-day mortality for patients with E coli or Klebsiella pneumoniae bloodstream infection and ceftriaxone resistance: A randomized clinical trial. JAMA 2018, 320, 984–994. [Google Scholar] [CrossRef] [Green Version]
  43. Tamma, P.D.; Aitken, S.L.; Bonomo, R.A.; Mathers, A.J.; van Duin, D.; Clancy, C.J. Infectious Diseases Society of America Guidance on the Treatment of Extended-Spectrum β-lactamase Producing Enterobacterales (ESBL-E), Carbapenem-Resistant Enterobacterales (CRE), and Pseudomonas aeruginosa with Difficult-to-Treat Resistance (DTR-P. aeruginosa). Clin. Infect. Dis. 2021, 72, e169–e183. [Google Scholar]
  44. Gatti, M.; Viaggi, B.; Rossolini, G.M.; Pea, F.; Viale, P. An Evidence-Based Multidisciplinary Approach Focused at Creating Algorithms for Targeted Therapy of BSIs, cUTIs, and cIAIs Caused by Enterobacterales in Critically Ill Adult Patients. Infect. Drug Resist. 2021, 14, 2461–2498. [Google Scholar] [CrossRef]
  45. Montravers, P.; Dupont, H.; Leone, M.; Constantin, J.M.; Mertes, P.M.; Société Française D’anesthésie et de Réanimation (Sfar); Société de Réanimation de Langue Française (SRLF); Laterre, P.F.; Misset, B.; Société de Pathologie Infectieuse de Langue Française (SPILF); et al. Guidelines for management of intra-abdominal infections. Anaesth. Crit. Care Pain Med. 2015, 34, 117–130. [Google Scholar] [CrossRef] [Green Version]
  46. Heizmann, W.R.; Löschmann, P.A.; Eckmann, C.; Von Eiff, C.; Bodmann, K.F.; Petrik, C. Clinical efficacy of tigecycline used as monotherapy or in combination regimens for complicated infections with documented involvement of multiresistant bacteria. Infection 2015, 43, 37–43. [Google Scholar] [CrossRef] [Green Version]
  47. McGovern, P.C.; Wible, M.; El-Tahtawy, A.; Biswas, P.; Meyer, R.D. All-cause mortality imbalance in the tigecycline phase 3 and 4 clinical trials. Int. J. Antimicrob. Agents 2013, 41, 463–467. [Google Scholar] [CrossRef] [Green Version]
  48. Bassetti, M.; McGovern, P.C.; Wenisch, C.; Meyer, R.D.; Yan, J.L.; Wible, M.; Rottinghaus, S.T.; Quintana, A. Clinical response and mortality in tigecycline complicated intra-abdominal infection and complicated skin and soft-tissue infection trials. Int. J. Antimicrob. Agents 2015, 46, 346–350. [Google Scholar] [CrossRef] [Green Version]
  49. Scott, L.J. Eravacycline: A Review in Complicated Intra-Abdominal Infections. Drugs 2019, 79, 315–324. [Google Scholar] [CrossRef] [Green Version]
  50. Solomkin, J.; Hershberger, E.; Miller, B.; Popejoy, M.; Friedland, I.; Steenbergen, J.; Yoon, M.; Collins, S.; Yuan, G.; Barie, P.S. Ceftolozane/Tazobactam plus metronidazole for complicated intra-abdominal infections in an era of multidrug resistance: Results from a randomized, double-blind, phase 3 trial (ASPECT-cIAI). Clin. Infect. Dis. 2015, 60, 1462–1471. [Google Scholar] [CrossRef] [Green Version]
  51. Mazuski, J.E.; Gasink, L.B.; Armstrong, J.; Broadhurst, H.; Stone, G.G.; Rank, D.; Llorens, L.; Newell, P.; Pachl, J. Efficacy and safety of ceftazidime-avibactam plus metronidazole versus meropenem in the treatment of complicated intra-abdominal infection: Results from a randomized, controlled, double-blind, phase 3 program. Clin. Infect. Dis. 2016, 62, 1380–1389. [Google Scholar] [CrossRef] [Green Version]
  52. Nordmann, P.; Cuzon, G.; Naas, T. The real threat of Klebsiella pneumoniae carbapenemase-producing bacteria. Lancet Infect. Dis. 2009, 9, 228–236. [Google Scholar] [CrossRef]
  53. Lübbert, C.; Rodloff, A.C.; Laudi, S.; Simon, P.; Busch, T.; Mössner, J.; Bartels, M.; Kaisers, U.X. Lessons learned from excess mortality associated with Klebsiella pneumoniae carbapenemase 2-producing K. pneumoniae in liver transplant recipients. Liver Transpl. 2014, 20, 736–738. [Google Scholar] [CrossRef]
  54. Tzouvelekis, L.S.; Markogiannakis, A.; Piperaki, E.; Souli, M.; Daikos, G.L. Treating infections caused by carbapenemase-producing Enterobacterales. Clin. Microbiol. Infect. 2014, 20, 862–872. [Google Scholar] [CrossRef]
  55. Munoz-Price, L.S.; Poirel, L.; Bonomo, R.A.; Schwaber, M.J.; Daikos, G.L.; Cormican, M.; Cornaglia, G.; Garau, J.; Gniadkowski, M.; Hayden, M.K.; et al. Clinical epidemiology of the global expansion of Klebsiella pneumoniae carbapenemases. Lancet Infect. Dis. 2013, 13, 785–796. [Google Scholar] [CrossRef] [Green Version]
  56. Van Duin, D.; Lok, J.J.; Earley, M.; Cober, E.; Richter, S.S.; Perez, F.; Salata, R.A.; Kalayjian, R.C.; Watkins, R.R.; Doi, Y.; et al. Colistin versus ceftazidime-avibactam in the treatment of infections due to carbapenem-resistant Enterobacterales. Clin. Infect. Dis. 2018, 66, 163–171. [Google Scholar] [CrossRef] [Green Version]
  57. Castón, J.J.; Lacort-Peralta, I.; Martín-Dávila, P.; Loeches, B.; Tabares, S.; Temkin, L.; Torre-Cisneros, J.; Paño-Pardo, J.R. Clinical efficacy of ceftazidime/avibactam versus other active agents for the treatment of bacteremia due to carbapenemase-producing Enterobacterales in hematologic patients. Int. J. Infect. Dis. 2017, 59, 118–123. [Google Scholar] [CrossRef] [Green Version]
  58. Tumbarello, M.; Trecarichi, E.M.; Corona, A.; De Rosa, F.G.; Bassetti, M.; Mussini, C.; Menichetti, F.; Viscoli, C.; Campoli, C.; Venditti, M.; et al. Efficacy of ceftazidime-avibactam salvage therapy in patients with infections caused by Klebsiella pneumoniae carbapenemase-producing K. pneumoniae. Clin. Infect. Dis. 2019, 68, 355–364. [Google Scholar] [CrossRef] [Green Version]
  59. Shields, R.K.; Nguyen, M.H.; Chen, L.; Press, E.G.; Potoski, B.A.; Marini, R.V.; Doi, Y.; Kreiswirth, B.N.; Clancy, C.J. Ceftazidime-Avibactam is superior to other treatment regimens against carbapenem-resistant Klebsiella pneumoniae bacteremia. Antimicrob. Agents Chemother. 2017, 61, 8. [Google Scholar] [CrossRef] [Green Version]
  60. Temkin, E.; Torre-Cisneros, J.; Beovic, B.; Benito, N.; Giannella, M.; Gilarranz, R.; Jeremiah, C.; Loeches, B.; Machuca, I.; Jiménez-Martín, M.J.; et al. Ceftazidime-Avibactam as salvage therapy for infections caused by carbapenem-resistant organisms. Antimicrob. Agents Chemother. 2017, 61, 2. [Google Scholar] [CrossRef] [Green Version]
  61. King, M.; Heil, E.; Kuriakose, S.; Bias, T.; Huang, V.; El-Beyrouty, C.; McCoy, D.; Hiles, J.; Richards, L.; Gardner, J.; et al. Multicenter study of outcomes with ceftazidime-avibactam in patients with carbapenem-resistant Enterobacterales infections. Antimicrob. Agents Chemother. 2017, 61, 7. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  62. Wunderink, R.G.; Giamarellos-Bourboulis, E.J.; Rahav, G.; Rahav, G.; Mathers, A.J.; Bassetti, M.; Vazquez, J.; Cornely, O.A.; Solomkin, J.; Bhowmick, T.; et al. Effect and safety of meropenem-vaborbactam versus best-available therapy in patients with carbapenem-resistant Enterobacterales infections: The TANGO II randomized clinical trial. Infect. Dis. Ther. 2018, 7, 439–455. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  63. Ackley, R.; Roshdy, D.; Meredith, J.; Minor, S.; Anderson, W.E.; Capraro, G.A.; Polk, C. Meropenem-Vaborbactam versus Ceftazidime-Avibactam for Treatment of Carbapenem-Resistant Enterobacterales Infections. Antimicrob. Agents Chemother. 2020, 64, 5. [Google Scholar] [CrossRef]
  64. Alosaimy, S.; Jorgensen, S.C.J.; Lagnf, A.M.; Morrisette, T.; Scipione, M.R.; Zhao, J.J.; Jorgensen, S.C.; Mynatt, R.; Carlson, T.J.; Jo, J.; et al. Real-world multicenter analysis of clinical outcomes and safety of meropenem-vaborbactam in patients treated for serious gram-negative bacterial infections. Open Forum Infect. Dis. 2020, 7, ofaa051. [Google Scholar] [CrossRef] [PubMed]
  65. Motsch, J.; Murta de Oliveira, C.; Stus, V.; Köksal, I.; Lyulko, O.; Boucher, H.W.; Kaye, K.S.; File, T.M.; Brown, M.L.; Khan, I.; et al. RESTORE-IMI 1: A Multicenter, Randomized, Double-blind Trial Comparing Efficacy and Safety of Imipenem/Relebactam vs Colistin Plus Imipenem in Patients With Imipenem-nonsusceptible Bacterial Infections. Clin. Infect. Dis. 2020, 70, 1799–1808. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  66. Benchetrit, L.; Mathy, V.; Armand-Lefevre, L.; Bouadma, L.; Timsit, J.-F. Successful treatment of septic shock due to NDM-1-producing Klebsiella pneumoniae using ceftazidime/avibactam combined with aztreonam in solid organ transplant recipients: Report of two cases. Int. J. Antimicrob. Agents 2020, 55, 105842. [Google Scholar] [CrossRef] [PubMed]
  67. Falcone, M.; Daikos, G.L.; Tiseo, G.; Bassoulis, D.; Giordano, C.; Galfo, V.; Leonildi, A.; Tagliaferri, E.; Barnini, S.; Sani, S.; et al. Efficacy of Ceftazidime-avibactam Plus Aztreonam in Patients With Bloodstream Infections Caused by Metallo-β-lactamase-Producing Enterobacterales. Clin. Infect. Dis. 2021, 72, 1871–1878. [Google Scholar] [CrossRef]
  68. Hobson, C.A.; Bonacorsi, S.; Fahd, M.; Baruchel, A.; Cointe, A.; Poey, N.; Jacquier, H.; Doit, C.; Monjault, A.; Tenaillon, O.; et al. Successful Treatment of Bacteremia Due to NDM-1-Producing Morganella morganii with Aztreonam and Ceftazidime-Avibactam Combination in a Pediatric Patient with Hematologic Malignancy. Antimicrob. Agents Chemother. 2019, 63, 2. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  69. Bassetti, M.; Echols, R.; Matsunaga, Y.; Ariyasu, M.; Doi, Y.; Ferrer, R.; Lodise, T.P.; Naas, T.; Niki, Y.; Paterson, D.L.; et al. Efficacy and safety of cefiderocol or best available therapy for the treatment of serious infections caused by carbapenem-resistant Gram-negative bacteria (CREDIBLE-CR): A randomised, open-label, multicentre, pathogen-focused, descriptive, phase 3 trial. Lancet Infect. Dis. 2021, 21, 226–240. [Google Scholar] [CrossRef]
  70. Giurazza, R.; Mazza, M.C.; Andini, R.; Sansone, P.; Pace, M.C.; Durante-Mangoni, E. Emerging Treatment Options for Multi-Drug-Resistant Bacterial Infections. Life 2021, 11, 519. [Google Scholar] [CrossRef]
  71. Noskin, G.A. Vancomycin-resistant Enterococci: Clinical, microbiologic, and epidemiologic features. J. Lab. Clin. Med. 1997, 130, 14–20. [Google Scholar] [CrossRef]
  72. Morvan, A.C.; Hengy, B.; Garrouste-Orgeas, M.; Ruckly, S.; Forel, J.M.; Argaud, L.; Rimmelé, T.; Bedos, J.P.; Azoulay, E.; Dupuis, C.; et al. Impact of species and antibiotic therapy of enterococcal peritonitis on 30-day mortality in critical care-an analysis of the OUTCOMEREA database. Crit. Care 2019, 23, 307. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  73. Luo, X.; Li, L.; Xuan, J.; Zeng, Z.; Zhao, H.; Cai, S.; Huang, Q.; Guo, X.; Chen, Z. Risk Factors for Enterococcal Intra-Abdominal Infections and Outcomes in Intensive Care Unit Patients. Surg. Infect. 2021, 22, 845–853. [Google Scholar] [CrossRef] [PubMed]
  74. Sanders, J.M.; Tessier, J.M.; Sawyer, R.; Dellinger, E.P.; Miller, P.R.; Namias, N.; West, M.A.; Cook, C.H.; O’Neill, P.J.; Napolitano, L.; et al. Does Isolation of Enterococcus Affect Outcomes in Intra-Abdominal Infections? Surg. Infect. 2017, 18, 879–885. [Google Scholar] [CrossRef]
  75. Dupont, H.; Montravers, P.; Mohler, J.; Carbon, C. Disparate findings on the role of virulence factors of Enterococcus faecalis in mouse and rat models of peritonitis. Infect. Immun. 1998, 66, 2570–2575. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  76. Koch, S.; Hufnagel, M.; Theilacker, C.; Huebner, J. Enterococcal infections: Host response, therapeutic, and prophylactic possibilities. Vaccine 2004, 22, 822–830. [Google Scholar] [CrossRef]
  77. Fisher, K.; Phillips, C. The ecology, epidemiology and virulence of Enterococcus. Microbiology 2009, 155, 1749–1757. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  78. Chatterjee, I.; Iredell, J.R.; Woods, M.; Lipman, J. The implications of enterococci for the intensive care unit. Crit. Care Resusc. 2007, 9, 69–75. [Google Scholar]
  79. McBride, S.J.; Upton, A.; Roberts, S.A. Clinical characteristics and outcomes of patients with vancomycin-susceptible Enterococcus faecalis and Enterococcus faecium bacteraemia—A five-year retrospective review. Eur. J. Clin. Microbiol. Infect. Dis. 2010, 29, 107–114. [Google Scholar] [CrossRef] [PubMed]
  80. McGuinness, W.A.; Malachowa, N.; DeLeo, F.R. Vancomycin Resistance in Staphylococcus aureus. Yale J. Biol. Med. 2017, 90, 269–281. [Google Scholar] [PubMed]
  81. Riché, F.C.; Dray, X.; Laisné, M.J.; Matéo, J.; Raskine, L.; Sanson-Le Pors, M.J.; Payen, D.; Valleur, P.; Cholley, B.P. Factors associated with septic shock and mortality in generalized peritonitis: Comparison between community-acquired and postoperative peritonitis. Crit. Care 2009, 13, R99. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  82. Singer, M.; Deutschman, C.S.; Seymour, C.W.; Shankar-Hari, M.; Annane, D.; Bauer, M.; Bellomo, R.; Bernard, G.R.; Chiche, J.D.; Coopersmith, C.M.; et al. The Third International Consensus Definitions for Sepsis and Septic Shock (Sepsis-3). JAMA 2016, 315, 801–810. [Google Scholar] [CrossRef]
  83. Bone, R.C.; Balk, R.A.; Cerra, F.B.; Dellinger, R.P.; Fein, A.M.; Knaus, W.A.; Schein, R.M.; Sibbald, W.J. Definitions for sepsis and organ failure and guidelines for the use of innovative therapies in sepsis. Chest 1992, 101, 1644–1655. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  84. Levy, M.M.; Fink, M.P.; Marshall, J.C.; Abraham, E.; Angus, D.; Cook, D.; Cohen, J.; Opal, S.M.; Vincent, J.L.; Ramsay, G.; et al. 2001 SCCM/ESICM/ACCP/ATS/SIS International Sepsis Definitions Conference. Crit. Care Med. 2003, 31, 1250–1256. [Google Scholar] [CrossRef] [PubMed]
  85. Esteban, A.; Frutos-Vivar, F.; Ferguson, N.D.; Peñuelas, O.; Lorente, J.A.; Gordo, F.; Honrubia, T.; Algora, A.; Bustos, A.; García, G.; et al. Sepsis incidence and outcome: Contrasting the intensive care unit with the hospital ward. Crit. Care Med. 2007, 35, 1284–1289. [Google Scholar] [CrossRef] [PubMed]
  86. Rubio, I.; Osuchowski, M.F.; Shankar-Hari, M.; Skirecki, T.; Winkler, M.S.; Lachmann, G.; La Rosée, P.; Monneret, G.; Venet, F.; Bauer, M.; et al. Current gaps in sepsis immunology: New opportunities for translational research. Lancet Infect. Dis. 2019, 19, e422–e436. [Google Scholar] [CrossRef]
  87. Shani, V.; Muchtar, E.; Kariv, G.; Robenshtok, E.; Leibovici, L. Systematic review and meta-analysis of the efficacy of appropriate empiric antibiotic therapy for sepsis. Antimicrob. Agents Chemother. 2010, 54, 4851–4863. [Google Scholar]
  88. Bassetti, M.; Rello, J.; Blasi, F.; Goossens, H.; Sotgiu, G.; Tavoschi, L.; Zasowski, E.J.; Arber, M.R.; McCool, R.; Patterson, J.V.; et al. Systematic review of the impact of appropriate versus inappropriate initial antibiotic therapy on outcomes of patients with severe bacterial infections. Int. J. Antimicrob. Agents 2020, 56, 106184. [Google Scholar] [CrossRef] [PubMed]
  89. Weinberger, J.; Rhee, C.; Klompas, M. A critical analysis of the literature on time-to-antibiotics in suspected sepsis. J. Infect. Dis. 2020, 222, S110–S118. [Google Scholar] [CrossRef]
  90. Seymour, C.W.; Gesten, F.; Prescott, H.C.; Friedrich, M.E.; Iwashyna, T.J.; Phillips, G.S.; Lemeshow, S.; Osborn, T.; Terry, K.M.; Levy, M.M. Time to Treatment and Mortality during Mandated Emergency Care for Sepsis. N. Engl. J. Med. 2017, 376, 2235–2244. [Google Scholar] [CrossRef]
  91. Evans, L.; Rhodes, A.; Alhazzani, W.; Antonelli, M.; Coopersmith, C.M.; French, C.; Machado, F.R.; Mcintyre, L.; Ostermann, M.; Prescott, H.C.; et al. Surviving sepsis campaign: International guidelines for management of sepsis and septic shock 2021. Intensive Care Med. 2021, 47, 1181–1247. [Google Scholar] [CrossRef]
  92. Tabah, A.; Cotta, M.O.; Garnacho-Montero, J.; Schouten, J.; Roberts, J.A.; Lipman, J.; Tacey, M.; Timsit, J.-F.; Leone, M.; Zahar, J.R.; et al. A systematic review of the definitions, determinants, and clinical outcomes of antimicrobial de-escalation in the intensive care unit. Clin. Infect. Dis. 2016, 62, 1009–1017. [Google Scholar] [CrossRef] [Green Version]
  93. De Waele, J.J.; Schouten, J.; Beovic, B.; Tabah, A.; Leone, M. Antimicrobial de-escalation as part of antimicrobial stewardship in intensive care: No simple answers to simple questions—A viewpoint of experts. Intensive Care Med. 2020, 46, 236–244. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  94. Montravers, P.; Augustin, P.; Grall, N.; Desmard, M.; Allou, N.; Marmuse, J.P.; Guglielminotti, J. Characteristics and outcomes of anti-infective de-escalation during health care-associated intra-abdominal infections. Crit. Care 2016, 20, 83. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  95. Pea, F.; Viale, P. Bench-to-bedside review: Appropriate antibiotic therapy in severe sepsis and septic shock—Does the dose matter? Crit. Care 2009, 13, 214. [Google Scholar] [CrossRef] [Green Version]
  96. Lau, W.K.; Mercer, D.; Itani, K.M.; Nicolau, D.P.; Kuti, J.L.; Mansfield, D.; Dana, A. Randomized, open-label, comparative study of piperacillin-tazobactam administered by continuous infusion versus intermittent infusion for treatment of hospitalized patients with complicated intra-abdominal infection. Antimicrob. Agents Chemother. 2006, 50, 3556–3561. [Google Scholar] [CrossRef] [PubMed]
  97. Lipš, M.; Siller, M.; Strojil, J.; Urbánek, K.; Balík, M.; Suchánková, H. Pharmacokinetics of imipenem in critically ill patients during empirical treatment of nosocomial pneumonia: A comparison of 0.5-h and 3-h infusions. Int. J. Antimicrob. Agents 2014, 44, 358–362. [Google Scholar] [CrossRef]
  98. Zelenitsky, S.; Nash, J.; Weber, Z.; Iacovides, H.; Ariano, R. Targeted benefits of prolonged-infusion piperacillin-tazobactam in an in vitro infection model of Pseudomonas aeruginosa. J. Chemother. 2016, 28, 390–394. [Google Scholar] [CrossRef]
  99. Roberts, J.A.; Abdul-Aziz, M.H.; Davis, J.S.; Dulhunty, J.M.; Cotta, M.O.; Myburgh, J.; Bellomo, R.; Lipman, J. Continuous versus intermittent β-lactam infusion in severe sepsis. A meta-analysis of individual patient data from randomized trials. Am. J. Respir. Crit. Care Med. 2016, 194, 681–691. [Google Scholar] [CrossRef]
  100. Vardakas, K.Z.; Voulgaris, G.L.; Maliaros, A.; Samonis, G.; Fakagas, M.E. Prolonged versus short-term intravenous infusion of antipseudomonal β-lactams for patients with sepsis: A systematic review and meta-analysis of randomised trials. Lancet Infect. Dis. 2018, 18, 108–120. [Google Scholar] [CrossRef]
  101. Chen, H.; Yu, L.; Yu, Z. Prolonged infusion with β-lactam antibiotics for treatment of infection caused by non-susceptible bacteria: A study protocol for a systemic review and meta-analysis. BMJ Open 2019, 9, e027509. [Google Scholar] [CrossRef] [Green Version]
  102. Kondo, Y.; Ota, K.; Imura, H.; Hara, N.; Shime, N. Prolonged versus intermittent β-lactam antibiotics intravenous infusion strategy in sepsis or septic shock patients: A systematic review with meta-analysis and trial sequential analysis of randomized trials. J. Intensive Care 2020, 8, 77. [Google Scholar] [CrossRef]
  103. Hatala, R.; Dinh, T.; Cook, D.J. Once-daily aminoglycoside dosing in immunocompetent adults: A meta-analysis. Ann. Intern. Med. 1996, 124, 717–725. [Google Scholar] [CrossRef]
  104. Greenberg, J.A.; Hohmann, S.F.; Hall, J.B.; Kress, J.P.; David, M.Z. Validation of a method to identify immunocompromised patients with severe sepsis in administrative databases. Ann. Am. Thorac. Soc. 2016, 13, 253–258. [Google Scholar] [CrossRef] [Green Version]
  105. Coccolini, F.; Improta, M.; Sartelli, M.; Rasa, K.; Sawyer, R.; Coimbra, R.; Chiarugi, M.; Litvin, A.; Hardcastle, T.; Forfori, F.; et al. Acute abdomen in the immunocompromised patient: WSES, SIS-E, WSIS, AAST, and GAIS guidelines. World J. Emerg. Surg. 2021, 16, 40. [Google Scholar] [CrossRef]
Table
Table 1. Patients with community-acquired intra-abdominal infection without sepsis or septic shock.
Table 1. Patients with community-acquired intra-abdominal infection without sepsis or septic shock.
Empiric Antibiotic Regimens; Normal Renal Function
One of the following intravenous antibiotics:
  Amoxicillin/clavulanate 2.2 g q8h 1
  Ceftriaxone 2 g every q24h + metronidazole 500 mg q8h
  Cefotaxime 2 g every 8 h + metronidazole 500 mg q8h
  Piperacillin/tazobactam 4 g/0.5 g q6h 2
In patients with beta-lactam allergy, a fluoroquinolone-based regimen:
  Ciprofloxacin 400 mg every q8/12h + metronidazole 500 mg q8h
In patients with beta-lactam allergy, an aminoglycoside regimen:
  Amikacin 15–20 mg/kg q24h + metronidazole 500 q8h
In patients at high risk of infection with community-acquired ESBL-producing Enterobacterales, one of the following antibiotics:
  Tigecycline 100 mg LD, then 50 mg every q12h (carbapenem-sparing strategy)
  Ertapenem 1 g q24h
1 Its use should be avoided if Enterobacterales local rate of resistance >20%. 2 In patients with advanced age (70 years of age or greater); presence of malignant disease; major compromise of cardiovascular, hepatic, or renal function; and/or hypoalbuminemia.
Table
Table 2. Patients with community-acquired intra-abdominal infection with sepsis or septic shock.
Table 2. Patients with community-acquired intra-abdominal infection with sepsis or septic shock.
Empiric Antibiotic Regimens; Normal Renal Function
One of the following intravenous antibiotics:
  Piperacillin/tazobactam 6 g/0.75 g LD then 4 g/0.5 g q6h or 16 g/2 g by continuous infusion.
In patients with documented beta-lactam allergy, an aminoglycoside regimen:
  Amikacin 15–20 mg/kg q24h + metronidazole 500 mg q8h
In patients at high risk of infection with community-acquired ESBL-producing Enterobacterales, one of the following antibiotics:
  Meropenem 1 g q8h (only in patients with septic shock) 1
  Doripenem 500 mg q8h (only in patients with septic shock) 1
  Imipenem/cilastatin 500 mg q6h (only in patients with septic shock)
1 Meropenem and doripenem have no in vitro activity against enterococci that are susceptible to ampicillin.
Table
Table 3. Patients with hospital-acquired IAIs without sepsis or septic shock.
Table 3. Patients with hospital-acquired IAIs without sepsis or septic shock.
Empiric Antibiotic Regimens; Normal Renal Function
One of the following intravenous antibiotics:
  Tigecycline 100 mg LD, then 50 mg every 12 h (not active against P. aeruginosa)
  Eravacycline 1 mg/kg q12 h (not active against P. aeruginosa)
  + Piperacillin/tazobactam 4.5 q6h
In patients with documented beta-lactam allergy:
  Amikacin 15–20 mg/kg q24h
In patients with high risk for invasive candidiasis:
  + Fluconazole 800 mg LD then 400 mg every 24 h
Table
Table 4. Patients with hospital-acquired intra-abdominal infection with sepsis or septic shock.
Table 4. Patients with hospital-acquired intra-abdominal infection with sepsis or septic shock.
Empiric Antibiotic Regimens; Normal Renal Function
One of the following intravenous antibiotics:
  Meropenem 1 g q8h
  Doripenem 500 mg q8h
  Imipenem/cilastatin 500 mg q6h
  +
One of the following intravenous antibiotics:
  Vancomycin 25–30 mg/kg LD then 15–20 mg/kg/q8 h
  Teicoplanin 12 mg/kg every 12 h 3 LDs then 12 mg/kg q24 h
In patients with high risk for invasive candidiasis, add one of the following antifungal agents:
  Caspofungin 70 mg LD, then 50 mg q24h
  Anidulafungin 200 mg LD, then 100 q24h
  Micafungin 100 mg q24h
  Amphotericin B liposomal 3 mg/kg q24h
In patients with suspected or proven infection with difficult-to-treat 1 non-metallo-beta-lactamase-producing P. aeruginosa, consider the use of antibiotic combinations with:
  Ceftolozane/tazobactam (1.5 g q8h), ceftazidime-avibactam (2.5 g q8h), and imipenem/cilastatin-relebactam (1.25 g q6h)
In patients with suspected or proven infection with carbapenemase-producing K. pneumoniae and MDR (non-metallo-beta-lactamase-producing) P. aeruginosa, consider the use of antibiotic combinations with:
  Ceftazidime-avibactam (2.5 g q8h), meropenem-vaborbactam (4 g 8qh), and imipenem/cilastatin-relebactam (1.25 g q6h)
In patients with suspected or proven infection with metallo-beta-lactamase-producing bacteria (i.e., NDM, VIM, IMP), consider the use of antibiotic combinations with:
  Ceftazidime-avibactam (2.5 g q8h) + aztreonam (2 g q8h) or cefiderocol (2 g q8h)
In patients with suspected or proven infection with vancomycin-resistant enterococci (VRE)—including patients with previous enterococcal infection or colonisation, immunocompromised patients, patients with long ICU stay, or patients with recent vancomycin exposure—consider the use of antibiotic combinations with:
  Linezolid (600 q 12h) or daptomycin (10–12 mg/kg q24h) 2
1 Difficult-to-treat is defined as P. aeruginosa that exhibits no susceptibility to any of the following: piperacillin/tazobactam, ceftazidime, cefepime, aztreonam, meropenem, imipenem/cilastatin, ciprofloxacin, and levofloxacin. 2 Approved at the dosage of 4 mg/kg/24 h, it is currently used at higher dosages.
Table
Table 5. Patients with IAIs with known colonisation (infection) by KPC-producing Enterobacterales.
Table 5. Patients with IAIs with known colonisation (infection) by KPC-producing Enterobacterales.
Oriented Antibiotic Regimens; Normal Renal Function
One of the following intravenous antibiotics 1:
  Ceftazidime/avibactam 2.5 g q8h + tigecycline 100 mg LD, then 50 mg every 12 h
  Ceftazidime/avibactam 2.5 g q8h + metronidazole 500 mg q8h
  Meropenem/vaborbactam 4 g 8qh infused in three hours
  Imipenem/cilastatin/relebactam 1.25 g q6h
  +
One of the following intravenous antibiotics (not for combinations with tigecycline):
  Vancomycin 25–30 mg/kg LD then 15–20 mg/kg/q8 h
  Teicoplanin 12 mg/kg every 12 h 3 LDs then 12 mg/kg q24 h
In patients at high risk of invasive candidiasis, add one of the following antifungal agents:
  Caspofungin 70 mg LD, then 50 mg q24h
  Anidulafungin 200 mg LD, then 100 q24h
  Micafungin 100 mg q24h
  Amphotericin B liposomal 3 mg/kg q24h
KPC: Klebsiella pneumonia carbapenemase. 1 The microorganism is known to be sensitive to the chosen beta-lactam.
Table
Table 6. Patients with IAIs with known colonisation (infection) by MBL-producing Enterobacterales.
Table 6. Patients with IAIs with known colonisation (infection) by MBL-producing Enterobacterales.
Oriented Antibiotic Regimens; Normal Renal Function
One of the following intravenous antibiotics:
  Ceftazidime/avibactam 2.5 g q8h + aztreonam 2 g q8h + tigecycline 100 mg LD, then 50 mg every 12 h
  Ceftazidime/avibactam 2.5 g q8h + aztreonam 2 g q8h + metronidazole 500 mg q8h
  Cefiderocol 2 g q8h + tigecycline 100 mg LD, then 50 mg every 12 h
  Cefiderocol 2 g q8h + metronidazole 500 mg q8h
In patients at high risk of invasive candidiasis, add one of the following antifungal agents:
  Caspofungin 70 mg LD, then 50 mg q24h
  Anidulafungin 200 mg LD, then 100 q24h
  Micafungin 100 mg q24h
  Amphotericin B Liposomal 3 mg/kg q24h
MBL: metallo-beta-lactamase.
Table
Table 7. Patients with IAIs with known colonisation by MBL-producing P. aeruginosa.
Table 7. Patients with IAIs with known colonisation by MBL-producing P. aeruginosa.
Oriented Antibiotic Regimens; Normal Renal Function
One of the following intravenous antibiotics:
  Cefiderocol 2 g q8h + tigecycline 100 mg LD, then 50 mg every 12 h
  Cefiderocol 2 g q8h + metronidazole 500 mg q8h
  Meropenem 2 g q8h + fosfomycin 4 g q6h
  +
One of the following intravenous antibiotics (not for combinations with tigecycline or fosfomycin):
  Vancomycin 25–30 mg/kg LD then 15–20 mg/kg/q8 h
  Teicoplanin 12 mg/kg every 12 h 3 LDs then 12 mg/kg q24 h
In patients at high risk of invasive candidiasis, add one of the following antifungal agents:
  Caspofungin 70 mg LD, then 50 mg q24h
  Anidulafungin 200 mg LD, then 100 q24h
  Micafungin 100 mg q24h
  Amphotericin B liposomal 3 mg/kg q24h
MBL: metallo-beta-lactamase.
Table
Table 8. Patients with IAIs with known colonisation by carbapenem-resistant A. baumannii.
Table 8. Patients with IAIs with known colonisation by carbapenem-resistant A. baumannii.
Oriented Antibiotic Regimens; Normal Renal Function
One of the following intravenous antibiotics:
  Cefiderocol 2 g q8h + tigecycline 100 mg LD, then 50 mg q12h
  Cefiderocol 2 g q8h + metronidazole 500 mg q8h
  Fosfomycin 4 g q6h + ampicillin/sulbactam 6/3 g q8h
  +
One of the following intravenous antibiotics (not for combinations with tigecycline or fosfomycin):
  Vancomycin 25–30 mg/kg LD then 15–20 mg/kg/q8h
  Teicoplanin 12 mg/kg every 12 h 3 LDs then 12 mg/kg q24h
In patients at high risk of invasive candidiasis, add one of the following antifungal agents:
  Caspofungin 70 mg LD, then 50 mg q24h
  Anidulafungin 200 mg LD, then 100 q24h
  Micafungin 100 mg q24h
  Amphotericin B liposomal 3 mg/kg q24h
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Sartelli, M.; Cristini, F.; Coccolini, F.; Labricciosa, F.M.; Siquini, W.; Catena, F. A Proposal for a Classification Guiding the Selection of Appropriate Antibiotic Therapy for Intra-Abdominal Infections. Antibiotics 2022, 11, 1394. https://doi.org/10.3390/antibiotics11101394

AMA Style

Sartelli M, Cristini F, Coccolini F, Labricciosa FM, Siquini W, Catena F. A Proposal for a Classification Guiding the Selection of Appropriate Antibiotic Therapy for Intra-Abdominal Infections. Antibiotics. 2022; 11(10):1394. https://doi.org/10.3390/antibiotics11101394

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Sartelli, Massimo, Francesco Cristini, Federico Coccolini, Francesco Maria Labricciosa, Walter Siquini, and Fausto Catena. 2022. "A Proposal for a Classification Guiding the Selection of Appropriate Antibiotic Therapy for Intra-Abdominal Infections" Antibiotics 11, no. 10: 1394. https://doi.org/10.3390/antibiotics11101394

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