In-Silico Studies toward the Improvement of the Antibacterial Activity of Pristinamycin IIB †
Department of Chemistry, University Abou-Bekr Belkaid of Tlemcen/Laboratory of Catalysis and Synthesis in Organic Chemistry LCSCO, Tlemcen 13000, Algeria
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Author to whom correspondence should be addressed.
†
Presented at the 25th International Electronic Conference on Synthetic Organic Chemistry, 15–30 November 2021; Available online: https://ecsoc-25.sciforum.net/ .
Chem. Proc. 2022, 8(1), 13; https://doi.org/10.3390/ecsoc-25-11703
Published: 14 November 2021
(This article belongs to the Proceedings of The 25th International Electronic Conference on Synthetic Organic Chemistry)
Abstract
:Pristinamycin IIB (PIIB) is a potent antibiotic with limited use, due to some structural problems and also due to the bacterial resistance exhibited toward the antibiotic. A thorough study led to the design of novel analogues of PIIB, based on the introduction of a difluorostatone moiety. Herein, we describe the initial in silico studies toward these novel analogues using ADMET modeling of predictive models in order to compute the physicochemistry and estimate the pharmacokinetics, drug-likeness and medicinal chemistry friendliness of these newly designed analogues.
1. Introduction
The streptogramin antibiotics are naturally occurring compounds isolated from Streptomyces and are classified as A and B groups according to their basic primary structure [1].
The first antibiotic mixture of streptogramin antibiotics was isolated from the producer strain Streptomyces graminofaciens from a soil sample in Texas [2].
Natural Pristinamycin IIB- group A is among the most interesting antibiotics in the streptogramin family [3]. Nevertheless, it presents numerous problems related to its chemical structure, such as instability to most pHs, weak solubility in aqueous media and resistance exhibited by bacteria [4,5].
In order to improve its poor pharmacological characteristics as therapeutic agents and overcome resistance mechanisms, we have designed new analogues of Pristinamycin IIB, based most importantly on the introduction of fluorine atoms.
Following studies in the late 1990s that indicated that poor pharmacokinetics and toxicity were important causes of costly late-stage failures in drug development, it has become widely appreciated that data on absorption, distribution, metabolism, excretion (ADME) and toxicity (T) should be considered as early as possible in the drug discovery process [6].
Interestingly, SwissADME was recently introduced as a web-based tool for ADMET modeling and it presents one of the most practical tools recently developed for ADMET prediction [7].
SwissADME uses quantum mechanical methods to assess the potential for interaction between small molecules under consideration and proteins known to be involved in ADME processes, such as cytochrome P450s. Moreover, it enables the prediction of physicochemical properties, in addition to lipophilicity (logP) and water solubility (logS). PK models and drug-likeness filters are other features available in this tool. Additionally, medicinal chemistry alerts are given, such as PAINS, the Brenk structural alert [8], lead-likeness [9] and synthetic accessibility.
2. Discussion
Accordingly, we have started this investigation by selecting Pristinamycin IIB as our lead compound to which we introduced two fluorine atoms at C15, along with other modifications, hence providing several fluorinated analogues.
Subsequently, using some predictive models, we computed the physico-chemistry and estimated the pharmacokinetics, drug-likeness and medicinal chemistry friendliness of the newly designed analogues of Pristinamycin IIB.
Thus, we submitted Pristinamycin IIB along with its two lead analogues (Figure 1) to the online SwissADME (http://www.swissadme.ch/, accessed on 15 November 2021) for evaluation.
For each structure submitted to SwissADME, we obtained over 31 data, some of which we did not report in Table 1 for practical reasons (Table 1).
Our analysis indicated that the primarily designed molecules do not possess all the required drug-likeness, bioavailability, synthetic accessibility and ADMET features. Nevertheless, the data derived from the established study was employed in suggesting some new modifications in order to create other promising new analogues.
On the other side, our group has started the total synthesis of some fluorinated analogues. Our multistep synthetic approach relies on a convergent assembly of three main fragments using a few key reactions, namely a Wittig reaction, a Grubbs reaction, and a hydroxy, -difluoro API (Advanced Pharmaceutical Intermediate) synthesis.
3. Conclusions
At this stage, computational approaches are the only option for accessing information about ADMET properties, but it is also acceptable that the predictions are not perfect, which is a convergent opinion with others reported in the literature.
These primary studies and results obtained during this work encourage us to complete the synthesis of these novel antibiotic analogues and work towards further optimization of a clinical candidate.
Acknowledgments
The authors would like to thank the Algerian DGRSDT for the specific research budget allocated to this program.
References
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Figure 1.
Pristinamycin IIB with its two newly designed lead analogues.
Table 1.
SwissADME data.
| Pristinamycin IIB | Analogue 1 | Analogue 2 | |
|---|---|---|---|
| Physicochemical roperties | |||
| Formula | C28H37N3O7 | C28H35F2N3O7 | C28H33F2N5O6 |
| Molecular weight | 527.61 g/mol | 563.59 g/mol | 573.59 g/mol |
| No. heavy atoms | 38 | 40 | 41 |
| No. arom. heavy atoms | 5 | 5 | 11 |
| Fraction Csp | 0.54 | 0.54 | 0.50 |
| No. rotatable bonds | 1 | 1 | 1 |
| No. H-bond acceptors | 8 | 10 | 10 |
| No. H-bond donors | 2 | 2 | 2 |
| Molar Refractivity | 148.14 | 148.28 | 149.66 |
| TPSA | 139.04 Å2 | 139.04 Å2 | 143.72 Å2 |
| Lipophilicity | |||
| Consensus Log Po/w | 1.91 | 2.36 | 1.78 |
| Water Solubility | |||
| Log S (ESOL) | −4.64 | −5.32 | −5.29 |
| Solubility | 1.22 × 10−2 mg/mL; 2.31 × 10−5 mol/L | 2.70 × 10−3 mg/mL; 4.79 × 10−6 mol/L | 2.97 × 10−3 mg/mL; 5.17 × 10−6 mol/L |
| Class | Moderately soluble | Moderately soluble | Moderately soluble |
| Log S (Ali) | −4.93 | −5.70 | −5.46 |
| Solubility | 6.19 × 10−3 mg/mL; 1.17 × 10−5 mol/L | 1.13 × 10−3 mg/mL; 2.00 × 10−6 mol/L | 1.97 × 10−3 mg/mL; 3.43 × 10−6 mol/L |
| Class | Moderately soluble | Moderately soluble | Moderately soluble |
| Log S (SILICOS-IT) | −4.19 | −4.70 | −5.21 |
| Solubility | 3.38 × 10−2 mg/mL; 6.40 × 10−5 mol/L | 1.13 × 10−2 mg/mL; 2.01 × 10−5 mol/L | 3.50 × 10−3 mg/mL; 6.11 × 10−6 mol/L |
| Class | Moderately soluble | Moderately soluble | Moderately soluble |
| Pharmacokinetics | |||
| GI absorption | High | Low | Low |
| BBB permeant | No | No | No |
| P-gp substrate | Yes | Yes | Yes |
| CYP1A2 inhibitor | No | No | No |
| CYP2C19 inhibito | No | No | No |
| CYP2C9 inhibitor | No | No | No |
| CYP2D6 inhibitor | No | No | No |
| CYP3A4 inhibitor | No | Yes | No |
| Drug-likeness | |||
| Lipinski | Yes | Yes | No |
| Ghose | No | No | No |
| Veber | Yes | Yes | No |
| Egan | No | No | No |
| Muegge | Yes | Yes | Yes |
| Bioavailability Score | 0.55 | 0.55 | 0.17 |
| Medicinal Chemistry | |||
| PAINS | 0 alert | 0 alert | 0 alert |
| Brenk | 0 alert | 0 alert | 0 alert |
| Lead-likeness | No; 1 violation: MW > 350 | No; 1 violation: MW > 350 | No; 1 violation: MW > 350 |
| Synthetic accessibility | 6.92 | 6.97 | 6.88 |
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MDPI and ACS Style
Chebieb, A.; Ziani-Cherif, C.; Bellifa, K. In-Silico Studies toward the Improvement of the Antibacterial Activity of Pristinamycin IIB. Chem. Proc. 2022, 8, 13. https://doi.org/10.3390/ecsoc-25-11703
AMA Style
Chebieb A, Ziani-Cherif C, Bellifa K. In-Silico Studies toward the Improvement of the Antibacterial Activity of Pristinamycin IIB. Chemistry Proceedings. 2022; 8(1):13. https://doi.org/10.3390/ecsoc-25-11703
Chicago/Turabian StyleChebieb, Assia, Chewki Ziani-Cherif, and Khadidja Bellifa. 2022. "In-Silico Studies toward the Improvement of the Antibacterial Activity of Pristinamycin IIB" Chemistry Proceedings 8, no. 1: 13. https://doi.org/10.3390/ecsoc-25-11703
