Differences in Clinical Presentations of Omicron Infections with the Lineages BA.2 and BA.5 in Mecklenburg-Western Pomerania, Germany, between April and July 2022
by
,
Katja Verena Goller
1,*,
Juliane Moritz
1,
Janine Ziemann
1,
Christian Kohler
2,
Karsten Becker
2,†
,
Nils-Olaf Hübner
1,3,*,† and
the CoMV-Gen Study Group
‡ 1
Central Unit for Infection Control and Prevention, University Medicine Greifswald, 17475 Greifswald, Germany
2
Friedrich-Loeffler-Institute of Medical Microbiology, University Medicine Greifswald, 17475 Greifswald, Germany
3
Institute for Hygiene and Environmental Medicine, University Medicine Greifswald, 17475 Greifswald, Germany
*
Authors to whom correspondence should be addressed.
†
These authors contributed equally to this work.
‡
The CoMV-Gen Study Group are listed in the acknowledgements
Viruses 2022, 14(9), 2033; https://doi.org/10.3390/v14092033
Submission received: 8 August 2022
/
Revised: 2 September 2022
/
Accepted: 8 September 2022
/
Published: 13 September 2022
(This article belongs to the Special Issue What SARS-CoV-2 Variants Have Taught Us: Evolutionary Challenges of RNA Viruses)
Abstract
:Knowledge on differences in the severity and symptoms of infections with the SARS-CoV-2 Omicron variants BA.2 (Pango lineage B.1.529.2) and BA.5 (Pango lineage B.1.529.5) is still scarce. We investigated epidemiological data available from the public health authorities in Mecklenburg-Western Pomerania, Northeast Germany, between April and July 2022 retrospectively. Comparative analyses revealed significant differences between recorded symptoms of BA.2 and BA.5 infected individuals and found strong correlations of associations between symptoms. In particular, the symptoms ‘chills or sweating’, ‘freeze’ and ‘runny nose’ were more frequently reported in BA.2 infections. In contrast, ‘other clinical symptoms’ appeared more frequently in Omicron infections with BA.5. However, the results obtained in this study provide no evidence that BA.5 has a higher pathogenicity or causes a more severe course of infection than BA.2. To our knowledge, this is the first report on clinical differences between the current Omicron variants BA.2 and BA.5 using public health data. Our study highlights the value of timely investigations of data collected by public health authorities to gather detailed information on the clinical presentation of different SARS-CoV-2 subvariants at an early stage.
1. Introduction
Starting in December 2021 and ongoing until July 2022, infections with the Severe Acute Respiratory Syndrome Virus 2 (SARS-CoV-2) in Germany have mainly been caused by the Omicron variant (Phylogenetic Assignment of Named Global Outbreak (Pango) lineage: B.1.1.529) and its subvariants BA.1, BA.2, BA.3, BA.4 and BA.5, including their respective sub-lineages [1]. In December 2021, the Omicron subvariant BA.2 was reported for the first time in Germany [1,2]. Since then, it has rapidly replaced the Omicron subvariant BA.1 that had been dominating until then and was the dominant variant by the end of February 2022 [1]. Concurrently, by the end of February 2022, the Omicron variant BA.5, first detected in April 2022 in South-Africa where it was responsible for a fifth wave between April and June 2022 [3,4], appeared in Germany [1]. The BA.5 variant increased rapidly and became the dominating variant in Germany by calendar week 23 (June 2022) [1].
Little is known about differences in the severity of disease between BA.2 and BA.5 infections. However, a study in animals recently suggested that BA.4 and BA.5 may be more pathogenic than BA.2 [5], and there is also evidence that the Omicron variants BA.4 and BA.5 exhibit a higher transmissibility than BA.2 [6].
Interestingly, to the best of our knowledge, differences in clinical presentations between the currently circulating Omicron variants BA.2 and BA.5 have not yet been reported on the basis of public health data. We therefore conducted a comparative analysis between BA.2 and BA.5 lineages using official reporting data from the public health authorities from the German federal state Mecklenburg-Western Pomerania.
2. Materials and Methods
In order to investigate differences in symptoms caused by infections with the Omicron lineages of BA.2 and BA.5, including their respective sub-lineages, data available from the public health authorities from the federal state Mecklenburg-Western Pomerania, Germany, were used. For the German federal state of Mecklenburg-Western Pomerania, the CoMV-Gen Study Group (www.comv-gen.de (accessed on 8 August 2022)) is entrusted by the state government with monitoring the circulating SARS-CoV-2 -variants in collaboration with local diagnostic laboratories and public health authorities. On behalf of the state government, the CoMV-Gen project’s mission is conducting the SARS-CoV-2 variant surveillance in Mecklenburg-Western Pomerania, including gathering genetic information from target PCRs as well as from whole genome sequencing analyses in collaboration with local diagnostic laboratories, and connecting these with epidemiological data available from the public health authorities. All confirmed positive cases recorded between 25 April and 13 July 2022 (covering twelve calendar weeks) in the public health surveillance system (Surveillance Outbreak Response Management and Analysis System (SORMAS) [7]) by the public health authorities from Mecklenburg-Western Pomerania were analyzed retrospectively. Data on symptoms were mainly collected by structured self-reporting questionnaires, and to a lesser extent, from interviews with the cases. Data from individuals that were notified as being infected by Omicron were collected. All cases reported as being infected by Omicron BA.2 or BA.5 lineages up to 13 July 2022 were considered for analyses. According to the standardized and cross-sectional German Corona Consensus Dataset (GECCO) [8] for research, symptoms relevant to COVID-19 were filtered out and frequencies were compared. In order to investigate the infection status across the years of age of the positive cases, five age groups in 20-year intervals were defined: 0–19, 20–39, 40–59, 60–79 and 80 and more years of age.
Ethical approval was granted by the ethics committee of the University of Greifswald, Germany (BB 125/21). Only anonymized aggregated data are shown in this manuscript and only symptomatic cases were used to compare symptoms when the exact lineages were assigned and reported in the system either as BA.2 or BA.5.
Statistical analyses were conducted by using SPSS 28.0 (IBM SPSS Statistics for Windows, Version 28.0. Armonk, NY, USA: IBM Corp.). For comparative analyses, Pearson’s chi-square tests were conducted, and the 95% confidence intervals (CI95) were determined A p-value of 0.05 was considered statistically significant. In order to analyze correlations between symptoms for both variants, non-parametric Spearman Rho correlation coefficients were determined for symptoms that occurred with a minimum overall frequency of 10% of cases.
3. Results
In total, 1027 cases with confirmed Omicron infections were reported in SORMAS during the study period (Figure 1). Of those, 607 cases were deposited as Omicron-positive in SORMAS but were not assigned to a specific sub-lineage, while 405 cases were characterized as BA.2 (n = 246) or BA.5 (n = 159), respectively. Fifteen cases belonged to other Omicron lineages including BA.1 (six cases) and BA.4 (nine cases). These 15 cases, as well as the unassigned cases, were excluded from the analyses.
Information on infection status per age group, sex, symptomatic and vaccination status are summarized in Table 1. Statistical analyses revealed no significant differences between the age groups, sex and vaccination status of BA.2 and BA.5 cases (Table 1). Within the BA.2 cases 124 individuals (50.1%), and of the BA.5 cases 69 individuals (43.3%) reported one or more symptoms (Pearson’s chi square statistics: p = 0.561).
A summary of the statistical analyses including CI95 intervals for each symptom and results from Pearson’s chi-square statistics are given in Table 2. No records for ‘acute respiratory distress syndrome’, ‘respiratory insufficiency/assisted ventilation’ and ‘oxygen saturation < 94%’ were given.
The absolute and relative frequency of the symptoms of cases of our study population either infected with BA.2 or BA.5 are additionally shown in Figure 2. Altogether, 21 specific symptoms (according to the GECCO-criteria [8]) are of relevance for COVID-19 infections and the content of the questionnaire. The most prominent symptoms reported in BA.2 as well as BA.5 cases were respiratory symptoms such as ‘runny nose’, ‘cough’ and ‘pharyngitis’. On the other hand, severe symptoms such as ‘acute respiratory distress syndrome’, ‘oxygen saturation below 94%’ and ‘respiratory insufficiency that needs assisted ventilation’ were not reported for both variants.
However, the Omicron BA.2 and BA.5 lineages also showed marked differences in the frequency of various symptoms, as shown in Table 2 and Figure 2. Significant differences in symptoms ‘chills or sweating’ and ‘freeze’ between BA.2 and BA.5 infections were observed. These symptoms were more frequently notified from individuals infected with BA.2 (‘chills or sweating’: p = 0.012; 17.7%, CI95: 11.8%–25.2%; ‘freeze’: p = 0.011; 23.4%; CI95: 16.6%–31.4%) than from BA.5 cases (‘chills or sweating’: 4.3%, CI95: 1.2–11.1%; ‘freeze’: 8.7%; CI95: 3.7–17.0%), with 88.7% of BA.2 cases more frequently reporting ‘runny nose’ (p = 0.023; CI95: 82.3–93.4%) than BA.5 cases (75.4%; CI95: 64.3–84.3%). In contrast, BA.5 cases significantly more often reported ‘other symptoms’ (p < 0.001; 58.0%, CI95: 46.2–69.1%) than BA.2 cases (31.5%, CI95: 23.8–40.0%). ‘Other symptoms’ included a wide range of symptoms such as ‘dullness’, ‘exhaustion, ‘fatigue’, ‘dizziness’ among others that are all not items in the GECCO catalogue. This might indicate a more elaborated set of symptoms reported from BA.5 cases.
Correlations between symptoms for both variants are shown in Table 3.
As shown in Table 3, ‘loss of smell’ was strongly correlated with ’loss of taste’ (Spearman Rho = 0.571, p < 0.01); ‘freeze’ was strongly correlated with ‘chills or sweating’ (Spearman Rho = 0.579, p < 0.01), as well as with ’muscle or body aches’ (Spearman Rho = 0.328, p < 0.01); and ‘headache’ was correlated to ‘runny nose’ associated with ‘cough’ (Spearman Rho = 0.334, p < 0.01).
4. Discussion
In this study, we conducted a comparative analysis of the clinical presentations between the Omicron BA.2 and BA.5 lineages, including their respective sub-lineages, using official reporting data from the public health authorities of the Germany federal state Mecklenburg-Western Pomerania. To the best of our knowledge, this is the first time that the differences in the clinical presentations between these two current Omicron lineages have been reported using public health data.
Both sub-lineages showed a comparable severity of infection with approximately 50% of cases being symptomatic. Overall, the symptoms ‘runny nose’, ‘cough’, ‘sore throat’ and ‘headache’ were most often reported by symptomatic cases in both variants, while ‘pneumonia’ and other symptoms of a severe course of the disease were rare or not reported. However, the BA.2 and BA.5 lineages showed that differences in the frequency of certain symptoms—e.g., ‘other symptoms’ that are not part of the GECCO list of relevance for COVID-19 infections—were reported more frequently from BA.5 than from BA.2 cases. In contrast, the symptoms ‘chills or sweating’, ‘freeze’ and ‘runny nose’ were more frequently reported in BA.2 cases. This fits well with the literature, with ‘headache’, ‘runny nose’, ‘sore throat’, ‘sneezing’, ‘persistent cough’ and ‘fever’ as the most prominent symptoms reported for COVID-19 infections [9].
Our analysis shows some strong correlations between symptoms. Some of these correlations can be explained by the fact that they are part of the respiratory symptom cluster [10], and some are clearly distinguishable but closely related, such as ‘loss of smell’ and ‘loss of taste’, respectively. Others can be explained by the fact that they are difficult for patients to distinguish, e.g., ‘freeze’ and ‘chills or sweating’, and some can be interpreted as a distinctive clinical course, e.g., ‘chills or sweating’ and ’muscle or body aches’. Other studies most prominently reported SARS-CoV-2 symptoms such as ‘loss of smell’ and ‘loss of taste’, mainly when associated with ‘fever’, and ‘cough’ in association with ‘shortness of breath’ and ‘chest pain’ [10]. However, different SARS-CoV-2 variants are known to exhibit different symptoms and influence the course of infections [2,11,12]. For BA.2, the European Centre for Disease Prevention and Control (ECDC) reports reduced evidence and for BA.5 no evidence for the impact on severity so far [13]. However, different variants and sub-variants have genetically determined differences that have been shown to correlate with different clinical features and outcomes [5,11].
Our study has several limitations that should be considered for the interpretation: First, the estimated differences in symptoms between the BA.2 and BA.5 lineages could be biased due to a low incidence situation at the beginning of a new wave. Second, the database provided by SORMAS is mainly based on self-reports of the patients who were either interviewed by the public health authorities staff or filled in standardized questionnaires on their own. In particular, the recording of symptoms depends on the timing of the query, the patient’s physical condition and their willingness to provide information. As the public health departments and the use of SORMAS is decentralized, the way in which data were collected (either by interview or questionnaire) may have some differences between counties and over time. Although response is mandatory, it is quite possible that, for example, severe cases who were too ill to answer the questions were not fully recorded, as hospital record data can, but which is not systematically used. Since the questioning is one-time after the notification date, it is also conceivable that, depending on the day of the response of the patient, not all symptoms were recorded; later, potential hospitalization during the course of infection may, thus, not have been reported. Another possible systematic error is the partial overlap of symptoms in the symptom categories. For example, the symptom ‘freeze’ resembles the symptom ‘chills’ and, thus, could be reported either in both categories or only in one. This could also explain the strong correlation between both symptoms. Third, only cases about which data on the Omicron lineage were present were included in the study. Therefore, only a small number (less than 5%) of confirmed cases could be included. This could aggravate the fact that, to date, many people use commercial self-testing systems when acquiring respiratory or other typical symptoms for COVID-19 infections and may, in some cases, not report their infection status to the public health authorities. Additionally, sub-lineages in the BA.2 and BA.5 groups were pooled in our analysis, despite the fact that the genetic heterogenicity amongst these sub-lineages steadily increased over the study period.
However, our study has some strengths: The data comprised official reporting data for a geographically distinct region and a manageable time frame. The Omicron lineages were well comparable in terms of age and sex structure, vaccination and frequency of symptomatic cases. Thus, it is not to be expected that external, undetected influences have significantly distorted the results.
In summary, our results provide no evidence that BA.5 has a higher pathogenicity than BA.2. However, approximately 50% of cases developed symptoms which could lead to sick leave. If the incidence is high, this could represent a significant social burden, especially in critical infrastructure and healthcare areas. Differences in symptoms between variants should continue to be closely monitored in order to identify symptomatic patterns early.
5. Conclusions
To our knowledge, we firstly report profound differences in symptoms between the Omicron lineages BA.2 and BA.5 based on public health data. Our results show some significant differences between the lineages but provide no evidence that BA.5 leads to a more severe course of disease than BA.2. Our study highlights the opportunities and challenges of analyzing routine data collected by the public health authorities in Germany to gather detailed information on variant behavior at an early stage.
The rapid identification of new variants or subvariants of SARS-CoV-2 is important for surveillance, in order to closely monitor the occurrence of infection and to enable initiating protective countermeasures. Timely investigations of public health data connected to confirmed circulating SARS-CoV-2 variants, including reported symptoms, enables the assessment of the current situation and the chance to react quickly to manage the pandemic.
Author Contributions
Conceptualization, N.-O.H., K.V.G. and K.B.; formal analysis, K.V.G., J.M. and N.-O.H.; resources, J.Z., C.K. and the CoMV-Gen Study Group; data curation, K.V.G., J.M. and J.Z.; writing—original draft preparation, K.V.G.; writing—review and editing, K.B., C.K., J.M., J.Z. and the CoMV-Gen Study Group; project administration, N.-O.H. and K.B. All authors have read and agreed to the published version of the manuscript.
Funding
This study was conducted in the framework of the CoMV-Gen project, and the study, as well as the APC, was funded by the Ministry of Social Affairs, Health and Sports of the Federal State Government of Mecklenburg-Western Pomerania, Germany. Number: CoMV-Gen.
Institutional Review Board Statement
Ethical approval was granted by the ethics committee of the University of Greifswald, Germany (BB 125/21; date of approval:10 August 2021).
Informed Consent Statement
Patient consent was waived since only anonymized aggregated data are shown.
Data Availability Statement
Not applicable.
Acknowledgments
We thank the public health authorities of Mecklenburg-Western Pomerania, Germany for providing us with data from the German surveillance system SORMAS and the collaborating diagnostic laboratories within the CoMV-Gen study group. The members of the CoMV-Gen Study Group are: Nils-Olaf Hübner (Central Unit for Infection Control and Prevention, University Medicine Greifswald, Greifswald, Germany; Institute for Hygiene and Environmental Medicine, University Medicine Greifswald, Germany); Karsten Becker (Friedrich Loeffler-Institute of Medical Microbiology, University Medicine Greifswald, Germany); Katja Verena Goller (Central Unit for Infection Control and Prevention, University Medicine Greifswald, Greifswald, Germany); Juliane Moritz (Central Unit for Infection Control and Prevention, University Medicine Greifswald, Greifswald, Germany); Janine Ziemann (Central Unit for Infection Control and Prevention, University Medicine Greifswald, Greifswald, Germany; KOMPASS e.V.—MRE-Netzwerk Mecklenburg-Vorpommern, Greifswald, Germany); Christian Kohler (Friedrich Loeffler-Institute of Medical Microbiology, University Medicine Greifswald, Germany); Jürgen Bohnert (Friedrich Loeffler-Institute of Medical Microbiology, University Medicine Greifswald, Germany); Lena Ulm (Friedrich Loeffler-Institute of Medical Microbiology, University Medicine Greifswald, Germany); Kathrin Zimmermann (Friedrich Loeffler-Institute of Medical Microbiology, University Medicine Greifswald, Germany); Lars Kaderali (Institute of Bioinformatics, University Medicine Greifswald, Greifswald, Germany); Ana Tzvetkova (Institute of Bioinformatics, University Medicine Greifswald, Greifswald, Germany); Martin Beer (Institute of Diagnostic Virology, Friedrich-Loeffler-Institut—Federal Research Institute for Animal Health, Greifswald-Insel Riems, Germany); Anne Pohlmann (Institute of Diagnostic Virology, Friedrich-Loeffler-Institut—Federal Research Institute for Animal Health, Greifswald-Insel Riems, Germany); Jacqueline King (Institute of Diagnostic Virology, Friedrich-Loeffler-Institut—Federal Research Institute for Animal Health, Greifswald-Insel Riems, Germany); Lina Stacker (Institute of Diagnostic Virology, Friedrich-Loeffler-Institut—Federal Research Institute for Animal Health, Greifswald-Insel Riems, Germany); Martina Littmann (LAGuS—Landesamt für Gesundheit und Soziales Mecklenburg-Vorpommern, Rostock, Germany); Tilo Sasse (LAGuS—Landesamt für Gesundheit und Soziales Mecklenburg-Vorpommern, Rostock, Germany); Kathrin Badstübner-Meeske (LAGuS—Landesamt für Gesundheit und Soziales Mecklenburg-Vorpommern, Rostock, Germany); Mandy Wietzke (LAGuS—Landesamt für Gesundheit und Soziales Mecklenburg-Vorpommern, Rostock, Germany); Elena Demihovska (LAGuS—Landesamt für Gesundheit und Soziales Mecklenburg-Vorpommern, Rostock, Germany); Ute Siering (District of Ludwigslust und Parchim, Ludwigslust, Germany); Robert Stach (District of Nordwestmecklenburg, Wismar, Germany); Gabriele Neumann (District of Nordwestmecklenburg, Wismar, Germany); Gerit Hübner (Municipality of Schwerin, Schwerin, Germany); Jasmin von Gadow (Municipality of Schwerin, Schwerin, Germany); Cornelia Ruhnau (District of Mecklenburgische Seenplatte, Neubrandenburg, Germany); Franz-Josef Stein (District of Mecklenburgische Seenplatte, Neubrandenburg, Germany); Kristin von der Oelsnitz (District of Rostock, Güstrow, Germany); Sylvia Krause (District of Rostock, Güstrow, Germany); Markus Schwarz (Municipality of Rostock, Rostock, Germany); Andi Friese (Municipality of Rostock, Rostock, Germany); Marlies Kühn (District of Vorpommern-Greifswald, Greifswald, Germany); Stefanie Hahn (District of Vorpommern-Greifswald, Greifswald, Germany); Marcel Neumeier (District of Vorpommern-Greifswald, Greifswald, Germany); Jörg Heusler (District of Vorpommern-Rügen, Stralsund, Germany); Kirstin Bengard (District of Vorpommern-Rügen, Stralsund, Germany); Egon Werle (Dietrich- Bonhoeffer-Klinikum Neubrandenburg (DBKNB) GmbH, Neubrandenburg, Germany); Eleonora Wasmund (Dietrich- Bonhoeffer-Klinikum Neubrandenburg (DBKNB) GmbH, Neubrandenburg, Germany); Lutz Briedigkeit (Helios Kliniken Schwerin, Schwerin, Germany); Kristian Meinck (IMD Labor Greifswald MVZ Labor Greifswald GmbH, Greifswald, Germany); Veronika Balau (IMD Labor Greifswald MVZ Labor Greifswald GmbH, Greifswald, Germany); Anja Kruggel (IMD Labor Greifswald MVZ Labor Greifswald GmbH, Greifswald, Germany); Mandy Wudtke (IMD Labor Greifswald MVZ Labor Greifswald GmbH, Greifswald, Germany); Ingo Neumann (Labor MVZ Westmecklenburg, Schwerin, Germany); Kirsten Gerst (LALLF—Landesamt für Landwirtschaft, Lebensmittelsicherheit und Fischerei Mecklenburg-Vorpommern, Rostock, Germany); Nele Matthes (LALLF—Landesamt für Landwirtschaft, Lebensmittelsicherheit und Fischerei Mecklenburg-Vorpommern, Rostock, Germany); Anja Balz (Medizinisches Labor Rostock, Rostock, Germany); Antje Lange (Medizinisches Labor Rostock, Rostock, Germany); Franziska Arnold (MVZ Martinsried GmbH, Martinsried, Germany); Oliver Wachter (MVZ Martinsried GmbH, Martinsried, Germany); Sedat Karadeniz (MVZ Martinsried GmbH, Martinsried, Germany); Christoph Kopp (MVZ Martinsried GmbH, Martinsried, Germany); Patricia Stunic (MVZ Martinsried GmbH, Martinsried, Germany); Bernhard Miller (MVZ Labor PD Volkmann und Kollegen Karlsruhe GbR, Karlsruhe, Germany); Fabian Ripp (MVZ Labor PD Volkmann und Kollegen Karlsruhe GbR, Karlsruhe, Germany); Barbara Hartmann (MVZ Labor PD Volkmann und Kollegen Karlsruhe GbR, Karlsruhe, Germany); Alisa Mitin (MVZ Labor PD Volkmann und Kollegen Karlsruhe GbR, Karlsruhe, Germany); Stephan Schaefer (MVZ Labor Limbach Vorpommern-Rügen GmbH, Stralsund, Germany); Yvonne Gerdes (MVZ Labor Limbach Vorpommern-Rügen GmbH, Stralsund, Germany); Philipp Warnke (University Medicine Rostock—Institut für Medizinische Mikrobiologie, Virologie und Hygiene, Rostock, Germany); and Moritz Jansson (University Medicine Rostock—Institut für Medizinische Mikrobiologie, Virologie und Hygiene, Rostock, Germany).
Conflicts of Interest
The authors declare no conflict of interest.
References
- Robert Koch Institut (RKI). Wöchentlicher Lagebericht des RKI zur Coronavirus-Krankheit-2019 (COVID-19). Available online: http://www.rki.de/DE/Content/InfAZ/N/Neuartiges_Coronavirus/Daten/VOC_VOI_Tabelle.html (accessed on 7 July 2022).
- Sievers, C.; Zacher, B.; Ullrich, A.; Huska, M.; Fuchs, S.; Buda, S.; Haas, W.; Diercke, M.; an der Heiden, M.; Kröger, S. SARS-CoV-2 Omicron variants BA.1 and BA.2 both show similarly reduced disease severity of COVID-19 compared to Delta, Germany, 2021 to 2022. Eurosurveillance 2022, 27, 2200396. [Google Scholar] [CrossRef] [PubMed]
- Tegally, H.; Moir, M.; Everatt, J.; Giovanetti, M.; Scheepers, C.; Wilkinson, E.; Subramoney, K.; Makatini, Z.; Moyo, S.; Amoako, D.G.; et al. Emergence of SARS-CoV-2 Omicron lineages BA.4 and BA.5 in South Africa. Nat. Med. 2022, 1–6. [Google Scholar] [CrossRef] [PubMed]
- Viana, R.; Moyo, S.; Amoako, D.G.; Tegally, H.; Scheepers, C.; Althaus, C.L.; Anyaneji, U.J.; Bester, P.A.; Boni, M.F.; Chand, M.; et al. Rapid epidemic expansion of the SARS-CoV-2 Omicron variant in southern Africa. Nature 2022, 603, 679–686. [Google Scholar] [CrossRef] [PubMed]
- Kimura, I.; Yamasoba, D.; Tamura, T.; Nao, N.; Oda, Y.; Mitoma, S.; Ito, J.; Nasser, H.; Zahradnik, J.; Uriu, K.; et al. Virological characteristics of the novel SARS-CoV-2 Omicron variants including BA.2.12.1, BA.4 and BA.5. bioRxiv 2022. [Google Scholar] [CrossRef]
- Cao, Y.; Yisimayi, A.; Jian, F.; Song, W.; Xiao, T.; Wang, L.; Du, S.; Wang, J.; Li, Q.; Chen, X.; et al. BA.2.12.1, BA.4 and BA.5 escape antibodies elicited by Omicron infection. Nature 2022, 608, 593–602. [Google Scholar] [CrossRef] [PubMed]
- Tom-Aba, D.; Silenou, B.C.; Doerrbecker, J.; Fourie, C.; Leitner, C.; Wahnschaffe, M.; Strysewske, M.; Arinze, C.C.; Krause, G. The Surveillance Outbreak Response Management and Analysis System (SORMAS): Digital Health Global Goods Maturity Assessment. JMIR Public Health Surveill. 2020, 6, e15860. [Google Scholar] [CrossRef] [PubMed]
- Sass, J.; Bartschke, A.; Lehne, M.; Essenwanger, A.; Rinaldi, E.; Rudolph, S.; Heitmann, K.U.; Vehreschild, J.J.; von Kalle, C.; Thun, S. The German Corona Consensus Dataset (GECCO): A standardized dataset for COVID-19 research in university medicine and beyond. BMC Med. Inform. Decis. Mak. 2020, 20, 341. [Google Scholar] [CrossRef] [PubMed]
- The ZOE Health Study. Omicron Symptoms: What Are They and How Long Do They Last? Available online: www.joinzoe.com/learn/omicron-symptoms (accessed on 8 July 2022).
- Dixon, B.E.; Wools-Kaloustian, K.; Fadel, W.F.; Duszynski, T.J.; Yiannoutsos, C.; Halverson, P.K.; Menachemi, N. Symptoms and symptom clusters associated with SARS-CoV-2 infection in community-based populations: Results from a statewide epidemiological study. PLoS ONE 2021, 16, e0241875. [Google Scholar] [CrossRef] [PubMed]
- Menni, C.; Valdes, A.M.; Polidori, L.; Antonelli, M.; Penamakuri, S.; Nogal, A.; Louca, P.; May, A.; Figueiredo, J.C.; Hu, C.; et al. Symptom prevalence, duration, and risk of hospital admission in individuals infected with SARS-CoV-2 during periods of omicron and delta variant dominance: A prospective observational study from the ZOE COVID Study. Lancet 2022, 399, 1618–1624. [Google Scholar] [CrossRef]
- Meo, S.A.; Meo, A.S.; Al-Jassir, F.F.; Klonoff, D.C. Omicron SARS-CoV-2 new variant: Global prevalence and biological and clinical characteristics. Eur. Rev. Med. Pharmacol. Sci. 2021, 25, 8012–8018. [Google Scholar] [CrossRef]
- European Centre for Disease Prevention and Control. Available online: https://www.ecdc.europa.eu/en/COVID-19/variants-concern (accessed on 18 July 2022).
Figure 1.
Sample size of the study population. In total, 405 assigned BA.2 and BA.5 cases were included in the analyses.
Figure 1.
Sample size of the study population. In total, 405 assigned BA.2 and BA.5 cases were included in the analyses.
Figure 2.
Relative frequency of the most prominent 18 symptoms of infected symptomatic BA.2 and BA.5 cases. * p values are given in squared brackets for significant results.
Figure 2.
Relative frequency of the most prominent 18 symptoms of infected symptomatic BA.2 and BA.5 cases. * p values are given in squared brackets for significant results.
Table 1.
Epidemiological characteristics and analyses on information from recorded BA.2 and BA.5 cases.
Table 1.
Epidemiological characteristics and analyses on information from recorded BA.2 and BA.5 cases.
| Characteristics | BA.2 | BA.5 | p Value 1 | ||||
|---|---|---|---|---|---|---|---|
| n | [%] | n | [%] | ||||
| Sex | Female | 126 | 51.2 | 96 | 60.4 | 0.135 | |
| Male | 118 | 48.0 | 61 | 38.4 | |||
| Unknown | 2 | 0.8 | 2 | 1.3 | |||
| Age groups | 0–19 | 25 | 10.2 | 13 | 8.2 | 0.759 | |
| 20–39 | 76 | 30.9 | 48 | 30.2 | |||
| 40–59 | 94 | 38.2 | 70 | 44.0 | |||
| 60–79 | 43 | 17.5 | 24 | 15.1 | |||
| 80+ | 7 | 2.8 | 3 | 1.9 | |||
| Unknown | 1 | 0.4 | 1 | 0.6 | |||
| Symptoms | Yes | 124 | 50.1 | 69 | 43.4 | 0.186 | |
| No | 122 | 49.9 | 90 | 56.6 | |||
| Vaccination 2 | Yes | 75 | 57.7 | 60 | 49.2 | 0.124 | |
| No | 42 | 32.3 | 54 | 44.3 | |||
| Unknown | 13 | 10 | 8 | 6.6 | |||
1p values are shown from Pearson’s chi square statistics. 2 No records from 174 cases.
Table 2.
Differences between reported symptoms from symptomatic BA.2 and BA.5 cases (CI, confidence interval (CI 95% [lower–upper]); Positive, positively reported; n.r., not reported.).
Table 2.
Differences between reported symptoms from symptomatic BA.2 and BA.5 cases (CI, confidence interval (CI 95% [lower–upper]); Positive, positively reported; n.r., not reported.).
| Symptom | Status | BA.2 | BA.5 | p-Value 1 | ||||
|---|---|---|---|---|---|---|---|---|
| n | % | CI 95 [%] | n | % | CI 95 [%] | |||
| Breathing difficulties/dyspnoea | Positive | 18 | 14.5 | [9.2–21.5] | 4 | 5.8 | [2.0–13.2] | 0.097 |
| n.r. | 106 | 85.5 | [78.5–90.8] | 65 | 94.2 | [86.8–98.0] | ||
| Chills or sweating | Positive | 22 | 17.7 | [11.8–25.2] | 3 | 4.3 | [1.2–11.1] | 0.012 |
| n.r. | 102 | 82.3 | [74.8–88.2] | 66 | 95.7 | [88.9–98.8] | ||
| Cough | Positive | 105 | 84.7 | [77.6–90.2] | 52 | 75.4 | [64.3–84.3] | 0.125 |
| n.r. | 19 | 15.3 | [9.8–22.4] | 17 | 24.6 | [15.7–35.7] | ||
| Diarrhea | Positive | 12 | 9.7 | [5.4–15.8] | 9 | 13 | [6.7–22.5] | 0.631 |
| n.r. | 112 | 90.3 | [84.2–94.6] | 60 | 87 | [77.5–93.3] | ||
| Fever | Positive | 43 | 34.7 | [26.7–43.3] | 34 | 49.3 | [37.7–60.9] | 0.065 |
| n.r. | 81 | 65.3 | [56.7–73.3] | 35 | 50.7 | [39.1–62.3] | ||
| Freeze | Positive | 29 | 23.4 | [16.6–31.4] | 6 | 8.7 | [3.7–17.0] | 0.011 |
| n.r. | 95 | 76.6 | [68.6–83.4] | 63 | 91.3 | [83.0–96.3] | ||
| Headache | Positive | 68 | 54.8 | [46.1–63.4] | 37 | 53.6 | [41.9–65.0] | 0.881 |
| n.r. | 56 | 45.2 | [36.6–53.9] | 32 | 46.4 | [35.0–58.1] | ||
| Increased heart rate/tachycardia | Positive | 12 | 9.7 | [5.4–15.8] | 3 | 4.3 | [1.2–11.1] | 0.264 |
| n.r. | 112 | 90.3 | [84.2–94.6] | 66 | 95.7 | [88.9–98.8] | ||
| Loss of smell | Positive | 15 | 12.1 | [7.2–18.7] | 15 | 21.7 | [13.3–32.5] | 0.097 |
| n.r. | 109 | 87.9 | [81.3–92.8] | 54 | 78.3 | [67.5–86.7] | ||
| Loss of taste | Positive | 25 | 20.2 | [13.8–27.9] | 17 | 24.6 | [15.7–35.7] | 0.585 |
| n.r. | 99 | 79.8 | [72.1–86.2] | 52 | 75.4 | [64.3–84.3] | ||
| Muscle or body aches | Positive | 40 | 32.3 | [24.5–40.8] | 28 | 40.6 | [29.6–52.4] | 0.273 |
| n.r. | 84 | 67.7 | [59.2–75.5] | 41 | 59.4 | [47.6–70.4] | ||
| Nausea | Positive | 8 | 6.5 | [3.1–11.8] | 6 | 8.7 | [3.7–17.0] | 0.774 |
| n.r. | 116 | 93.5 | [88.2–96.9] | 63 | 91.3 | [83.0–96.3] | ||
| Other symptoms 2 | Positive | 39 | 31.5 | [23.8–40.0] | 40 | 58.0 | [46.2–69.1] | <0.001 |
| n.r. | 85 | 68.5 | [60.0–76.2] | 29 | 42.0 | [30.9–53.8] | ||
| Pneumonia | Positive | 2 | 1.6 | [0.3–5.1] | 0 | 0 | [–] | 0.289 |
| n.r. | 122 | 98.4 | [94.9–99.7] | 69 | 100 | [–] | ||
| Rapid breathing/tachypnea | Positive | 2 | 1.6 | [0.3–5.1] | 2 | 2.9 | [0.6–9.0] | 0.618 |
| n.r. | 122 | 98.4 | [94.9–99.7] | 67 | 97.1 | [91.0–99.4] | ||
| Runny nose | Positive | 110 | 88.7 | [82.3–93.4] | 52 | 75.4 | [64.3–84.3] | 0.023 |
| n.r. | 14 | 11.3 | [6.6–17.7] | 17 | 24.6 | [15.7–35.7] | ||
| Severe feeling of sickness | Positive | 40 | 32.3 | [24.5–40.8] | 30 | 43.5 | [32.2–55.2] | 0.159 |
| n.r. | 84 | 67.7 | [59.2–75.5] | 39 | 56.5 | [44.8–67.8] | ||
| Sore throat/pharyngitis | Positive | 77 | 62.1 | [53.4–70.3] | 37 | 53.6 | [41.9–65.0] | 0.538 |
| n.r. | 47 | 37.9 | [29.7–46.6] | 32 | 46.4 | [35.0–58.1] | ||
1 In bold: significant p values are shown from Pearson’s chi square statistics. 2 ‘Other symptoms’ are explained in the text.
Table 3.
Non-parametric correlation between different symptoms of both BA.2 and BA.5 positive cases. Spearman-Rho correlation coefficients > 0.3. are given in bold.
Table 3.
Non-parametric correlation between different symptoms of both BA.2 and BA.5 positive cases. Spearman-Rho correlation coefficients > 0.3. are given in bold.
| Symptoms | |||||||||||||
|---|---|---|---|---|---|---|---|---|---|---|---|---|---|
| Chills or Sweating | Cough | Diarrhea | Breathing Difficulties/Dyspnea | Fever | Headache | Muscle or Body Aches | Rapid Breathing/Tachypnea | Runny Nose | Sore Throat/Pharyngitis | Loss of Taste | Loss of Smell | Freeze | |
| Chills or sweating | 1.000 | ||||||||||||
| Cough | 0.026 | 1.000 | |||||||||||
| Diarrhea | 0.063 | 0.082 | 1.000 | ||||||||||
| Breathing difficulties/dyspnea | 0.299 2 | 0.046 | 0.136 | 1.000 | |||||||||
| Fever | 0.095 | 0.064 | 0.191 2 | 0.107 | 1.000 | ||||||||
| Headache | 0.198 2 | 0.096 | 0.019 | 0.230 2 | 0.278 2 | 1.000 | |||||||
| Muscle or body aches | 0.232 2 | 0.047 | 0.125 | 0.179 1 | 0.174 1 | 0.414 2 | 1.000 | ||||||
| Rapid breathing/tachypnea | 0.161 1 | 0.07 | 0.066 | 0.291 2 | 0.179 1 | 0.133 | 0.121 | 1.000 | |||||
| Runny nose | 0.169 1 | 0.334 2 | 0.108 | 0.113 | −0.105 | 0.053 | −0.002 | 0.064 | 1.000 | ||||
| Sore throat/pharyngitis | 0.07 | 0.169 1 | 0.122 | 0.1 | 0.205 2 | 0.190 2 | 0.217 2 | −0.027 | 0.181 1 | 1.000 | |||
| Loss of taste | 0.096 | 0.059 | 0.219 2 | 0.127 | 0.109 | 0.079 | 0.242 2 | 0.188 2 | 0.094 | 0.107 | 1.000 | ||
| Loss of smell | 0.133 | 0.022 | 0.263 2 | 0.251 2 | 0.147 1 | 0.163 1 | 0.192 2 | 0.239 2 | 0.149 1 | 0.124 | 0.5712 | 1.000 | |
| Freeze | 0.5792 | 0.122 | 0.181 1 | 0.254 2 | 0.111 | 0.269 2 | 0.3282 | 0.12 | 0.206 2 | 0.009 | 0.045 | 0.021 | 1.000 |
1 Significant correlations p < 0.05. 2 Significant correlations p < 0.01.
Publisher’s Note: MDPI stays neutral with regard to jurisdictional claims in published maps and institutional affiliations. |
© 2022 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
Share and Cite
MDPI and ACS Style
Goller, K.V.; Moritz, J.; Ziemann, J.; Kohler, C.; Becker, K.; Hübner, N.-O.; the CoMV-Gen Study Group. Differences in Clinical Presentations of Omicron Infections with the Lineages BA.2 and BA.5 in Mecklenburg-Western Pomerania, Germany, between April and July 2022. Viruses 2022, 14, 2033. https://doi.org/10.3390/v14092033
AMA Style
Goller KV, Moritz J, Ziemann J, Kohler C, Becker K, Hübner N-O, the CoMV-Gen Study Group. Differences in Clinical Presentations of Omicron Infections with the Lineages BA.2 and BA.5 in Mecklenburg-Western Pomerania, Germany, between April and July 2022. Viruses. 2022; 14(9):2033. https://doi.org/10.3390/v14092033
Chicago/Turabian StyleGoller, Katja Verena, Juliane Moritz, Janine Ziemann, Christian Kohler, Karsten Becker, Nils-Olaf Hübner, and the CoMV-Gen Study Group. 2022. "Differences in Clinical Presentations of Omicron Infections with the Lineages BA.2 and BA.5 in Mecklenburg-Western Pomerania, Germany, between April and July 2022" Viruses 14, no. 9: 2033. https://doi.org/10.3390/v14092033
Note that from the first issue of 2016, this journal uses article numbers instead of page numbers. See further details here.
