Inflammatory Polymorphisms (IL-6 rs1800796, IL-10 rs1800896, TNF-α rs1800629, and IFITM3 rs12252) Are Not Associated with Post-COVID Symptoms in Previously Hospitalized COVID-19 Survivors
by
, , , , , , , , , and
César Fernández-de-las-Peñas
1,2,*,
Gema Díaz-Gil
3,
Antonio Gil-Crujera
3,
Stella M. Gómez-Sánchez
3,
Silvia Ambite-Quesada
1,
Juan Torres-Macho
4,5,
Pablo Ryan-Murua
4,
Ana I. Franco-Moreno
4,
Oscar J. Pellicer-Valero
6,
Lars Arendt-Nielsen
2,7,8 and
Rocco Giordano
2,9 1
Department of Physical Therapy, Occupational Therapy, Rehabilitation and Physical Medicine, Universidad Rey Juan Carlos, 28922 Alcorcón, Spain
2
Center for Neuroplasticity and Pain (CNAP), Sensory Motor Interaction (SMI), Department of Health Science and Technology, Faculty of Medicine, Aalborg University, DK-9220 Aalborg, Denmark
3
Research group GAMDES, Department of Basic Health Sciences, Universidad Rey Juan Carlos (URJC), 28933 Madrid, Spain
4
Department of Internal Medicine, Hospital Universitario Infanta Leonor-Virgen de la Torre, 28031 Madrid, Spain
5
Department of Medicine, School of Medicine, Universidad Complutense de Madrid, 28040 Madrid, Spain
6
Image Processing Laboratory (IPL), Universitat de València, Parc Científic, Paterna, 46100 València, Spain
7
Department of Gastroenterology & Hepatology, Mech-Sense, Clinical Institute, Aalborg University Hospital, DK-9000 Aalborg, Denmark
8
Steno Diabetes Center North Denmark, Clinical Institute, Aalborg University Hospital, DK-9000 Aalborg, Denmark
9
Department of Oral and Maxillofacial Surgery, Aalborg University Hospital, DK-9000 Aalborg, Denmark
*
Author to whom correspondence should be addressed.
Viruses 2024, 16(2), 275; https://doi.org/10.3390/v16020275
Submission received: 11 January 2024
/
Revised: 5 February 2024
/
Accepted: 8 February 2024
/
Published: 9 February 2024
(This article belongs to the Section Coronaviruses)
Abstract
:The aim of this study was to identify the association between four selected inflammatory polymorphisms with the development of long-term post-COVID symptoms in subjects who had been hospitalized due to SARS-CoV-2 infection during the first wave of the pandemic. These polymorphisms were selected as they are associated with severe COVID-19 disease and cytokine storm, so they could be important to prognoses post-COVID. A total of 408 (48.5% female, age: 58.5 ± 14.0 years) previously hospitalized COVID-19 survivors participated. The three potential genotypes of the following four single-nucleotide polymorphisms, IL-6 rs1800796, IL-10 rs1800896, TNF-α rs1800629, and IFITM3 rs12252, were obtained from non-stimulated saliva samples of the participants. The participants were asked to self-report the presence of any post-COVID symptoms (defined as symptoms that had started no later than one month after SARS-CoV-2 acute infection) and whether the symptoms persisted at the time of the study. At the time of the study (mean: 15.6, SD: 5.6 months after discharge), 89.4% of patients reported at least one post-COVID symptom (mean number of symptoms: 3.0; SD: 1.7). Fatigue (69.3%), pain (40.9%), and memory loss (27.2%) were the most prevalent post-COVID symptoms in the total sample. Overall, no differences in the post-COVID symptoms depending on the IL-6 rs1800796, IL-10 rs1800896, TNF-α rs1800629, and IFITM3 rs12252 genotypes were seen. The four SNPs assessed, albeit having been previously associated with inflammation and COVID-19 severity, did not cause a predisposition to the development of post-COVID symptoms in the previously hospitalized COVID-19 survivors.
1. Introduction
The identification of the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) virus, the agent responsible of the worldwide spread of coronavirus disease 2019 (COVID-19), was possible due to the analysis of samples from the lower respiratory tracts of infected individuals [1]. Several studies have focused on the specific viral mechanisms of SARS-CoV-2 infection, e.g., the entry pathways via different receptors (e.g., surface receptor for S1 of the angiotensin-converting enzyme 2 —ACE2—or transmembrane protease serine-2—TMPRSS2) [2] or the underlying mechanisms behind the pro-inflammatory response (i.e., cytokine storm) [3]. In fact, different types of cytokines play an important role in the pathophysiology of acute COVID-19. For instance, interleukin 6 (IL-6) and interleukin 10 (IL-10) exhibit a clear overproduction during an acute SARS-CoV-2 infection, particularly in patients with severe illness [4]. Thus, tumor necrosis factor-α (TNF-α) and interferon-induced transmembrane (IFITM) proteins have also been associated with severe COVID-19 and higher inflammatory states [5].
Different polymorphisms can account for the variability in expression of these pro-inflammatory cytokines [6]. For instance, genotyping of cytokine-related single-nucleotide polymorphisms (SNPs), e.g., IL-6 rs1800796 [7], IL-10 rs1800896 [8], TNF-α rs1800629 [9], and IFITM3 rs12252 [10], has shown them to underlie the differential viral virulence and severity of COVID-19. Looking at the research, most studies have investigated the potential role of SNPs at the acute phase of SARS-CoV-2 infection, focusing on the risk of developing the severe form of the COVID-19 illness [6,7,8,9,10]. Our understanding of the role of these SNPs in symptoms persisting after the acute phase of SARS-CoV-2 infection is still in its infancy.
A growing healthcare problem starting from the beginning of the COVID-19 outbreak has been the presence of long-lasting symptoms once the acute phase of SARS-CoV-2 infection has passed. The presence of symptoms after the acute phase of a SARS-CoV-2 infection is called long COVID [11] or post-COVID-19 condition [12]. The World Health Organization (WHO) adopted the term post-COVID-19 condition as defined by Soriano et al. [12]: “post-COVID-19 condition occurs in people with a history of probable or confirmed SARS-CoV-2 infection, usually three months from the onset of infection, with symptoms that last for at least two months and cannot be explained by an alternative medical diagnosis. Common symptoms include, but are not limited to, fatigue, shortness of breath (dyspnea), and cognitive dysfunction, and generally have an impact on everyday functioning” [12]. Post-COVID-19 condition or long COVID is a heterogeneous condition, and patients can experience a plethora of symptoms affecting multiple systems [13]. In fact, more than 100 symptoms affecting the cardiovascular, neurological, immune, respiratory, musculoskeletal, and gastrointestinal systems have been attributed to SARS-CoV-2 since the beginning of the pandemic [14]. With increasing evidence growing each week, and after three years of pandemic, recent meta-analyses have reported the presence of post-COVID symptoms one [15,16] or two [17] years after an acute SARS-CoV-2 infection in almost 25–30% of patients. Thus, the Global Burden of Disease Long COVID study (which included 1.2 million of subjects who had experienced an acute symptomatic SARS-CoV-2 infection) reported that 15% of COVID-19 survivors exhibit at least one post-COVID symptom one year after infection [18].
The underlying mechanisms explaining the presence of post-COVID symptoms are not completely understood, and different mechanisms have been proposed [19]. Long-lasting inflammation is proposed as a key mechanism contributing to the development of long COVID [20]. However, the evidence on the presence of inflammatory biomarkers in patients with post-COVID symptoms is still conflicting [21,22]. For instance, Lai et al. concluded that individuals with long COVID exhibit increased levels of 79 biomarkers but decreased levels of 29 biomarkers [21]. On the contrary, Williams et al. found reduced levels of IL-6, IL-2, IL-17, IL-13, and IL-4 in individuals with long COVID when compared with those without symptoms [22].
Due to the role of the inflammatory response in SARS-CoV-2 infection [23], it is possible that SNPs associated with the inflammatory response and associated with more severe illness can contribute to the development of long-lasting post-COVID symptoms. In a previous study, our research group observed that IL-6 rs1800796, IL-10 rs1800896, TNF-α rs1800629, and IFITM3 rs12252 SNPs, which are usually associated with the inflammatory and immune response, were not associated with a higher risk of developing post-COVID pain [24]. No data on the association of these four inflammatory SNPs with the presence of long-term post-COVID symptoms are available. Therefore, the aim of the current study was to investigate the association between the IL-6 rs1800796, IL-10 rs1800896, TNF-α rs1800629, and IFITM3 rs12252 polymorphisms and the presence of post-COVID symptoms in previously hospitalized COVID-19 survivors.
2. Methods
2.1. Participants
This study included individuals who had been hospitalized due to SARS-CoV-2 infection at four urban hospitals in Madrid (Spain) from March to May 2020 (first wave of the pandemic). The diagnosis of SARS-CoV-2 infection should have been confirmed using reverse transcription–polymerase chain reaction (RT–PCR) assay of a nasopharyngeal and oral swab sample, as well as clinical/radiological findings on hospital admission. Some of the participants in the current analysis were previously included in our previous study on pain [24], but the current data presented here are new, are based on a different sample, and have not previously been published. The study was approved by the Institutional Ethics Committees of all the institutions/hospitals involved (URJC0907202015920; HCSC20/495E, HSO25112020; HUFA 20/126; HUIL/092-20). All the participants provided their written informed consent prior to the collection of any data.
2.2. DNA Collection and Genotyping
The genotyping collection and management were the same as in our previous study and have been previously published [24]. Genotyping was obtained from unstimulated whole saliva samples collected from each subject, as previously described. The saliva samples were centrifuged at 3000 rpm for 15 min to obtain the cell sediment and stored at −20 °C until the analysis.
Genomic DNA was extracted from 500 mL of saliva using a MagMAX™ DNA Multi-Sample Ultra 2.0 Kit (Thermo Fisher Scientific Inc, Hemel Hempstead, Hertfordshire, UK). We extracted DNA using the KingFisher Flex purification robot (Thermo Fisher). The purity and concentration of the resulting DNA were assessed using Quant-iT™ PicoGreen™ dsDNA reagent (Thermo Fisher). The DNA was diluted to 5 ng/μL using 1× Tris-EDTA (TE) buffer (Sigma-Aldrich, Dorset, UK). The qPCR reaction mixtures of 10 μL contained a total of 10 ng of gDNA as a PCR template, 1× TaqMan Gene Expression PCR Master Mix, and 0.6× genotyping TaqMan probe assay [24].
A predesigned TaqMan® SNP Genotyping Assay (Thermo Fisher Scientific Inc, Hertfordshire, UK) was used for genotyping the SNPs using a real-time PCR reaction (RT–PCR). The real-time PCR plates were run using the QuantStudio 12K Flex system (Thermo Fisher) of the Genomics Unit (Madrid Science Park Foundation, Spain) under the standard conditions (95° for 10 min and 40 two-step cycles consisting of 95 °C for 15 s and 60 °C for 1 min) and analyzed using the Genotyping app in Thermo Fisher Cloud. Identification of each of the possible variants of each SNP was conducted using specific fluorescent dyes [24].
Three possible genotypes (C/G, C/C, G/G) associated with the IL-6 rs1800796 polymorphism were derived from a C→G substitution at the following sequence:
- ATGGCCAGGCAGTTCTACAACAGCC [C/G] CTCACAGGGGAGCCAGAACACAGA.
Three possible genotypes (C/C, T/C, T/T) associated with the IL-10 rs1800896 polymorphism were derived from a T→C substitution at the following sequence:
- TCCTCTTACCTATCCCTACTTCCCC [T/C] TCCCAAAGAAGCCTTAGTAGTGTTG.
Three possible genotypes (A/A, A/G, G/G) related to the TNF-α rs1800629 polymorphism were derived from an A→G substitution at the following sequence:
- GAGGCAATAGGTTTTGAGGGGCATG [A/G] GGACGGGGTTCAGCCTCCAGGGTCC.
Three possible genotypes (A/A, A/G, G/G) associated with the IFITM3 rs12252 polymorphism were derived from an A→G substitution at the following sequence:
- GCATCTCATAGTTGGGGGGCTGGCC [A/G] CTGTTGACAGGAGAGAAGAAGGTTT.
2.3. Collection Data
The demographic (age, gender, height, weight), clinical (medical comorbidities), and hospitalization (intensive care unit (ICU) admission, days in hospital) data were collected from medical records.
Participants who agreed to participate were scheduled for a face-to-face appointment with a healthcare professional. They were asked to self-report the presence of symptoms that appeared after hospitalization due to SARS-CoV-2 infection (no later than one month after) and whether the symptom(s) persisted at the time of the study. A list of symptoms (e.g., fatigue, dyspnea, anosmia, ageusia, brain fog, hair loss, pain, or concentration loss) was systematically used, although participants were free to report any symptom that they suffered from.
2.4. Statistical Analysis
The data were collected using STATA 16.1 and processed using Python’s library pandas 0.25.3. Means and standard deviation (SD) are presented for quantitative data and the number of cases (percentages) are presented for categorical data. Chi-squared (χ2) tests were applied to assess the deviation in the genotype distribution from Hardy–Weinberg equilibrium. Differences in the prevalence of post-COVID symptoms by the genotype frequencies of each polymorphism were analyzed using χ2 tests. Thus, differences in the continuous variables by the genotype frequencies of each polymorphism were analyzed using one-way-ANOVA tests. The Shapiro–Wilk test was used to assess the assumption of normality. For all inferences, the level of significance was set a priori at 0.05, with the p-values from all tests being corrected (Holm–Bonferroni correction).
3. Results
A total of 450 Hispanic/Latin patients who were hospitalized due to SARS-CoV-2 infection from March to May 2020 were initially invited to participate during the period (September 2021 to February 2022). A total of 42 (9.3%) patients were excluded as follows: 1, refused to participate (n = 19); 2, previous autoimmune pathology (n = 10); 3, pregnancy (n = 5); and 4, saliva sample compromised during genotyping analyses (n = 8). Finally, completed data from 408 (48.5% female, age: 58.5 ± 14.0 years) COVID-19 survivors were obtained with a follow-up period of 15.6 (SD 5.6) months after hospital discharge. At the time of the study, 365 (89.4%) patients reported post-COVID symptoms (mean symptoms number: 3.0; SD: 1.7). Fatigue (69.3%), pain (40.9%), and memory loss (27.2%) were the most prevalent post-COVID symptoms in the total sample (Table 1).
The genotype distributions did not deviate from those expected based on the Hardy–Weinberg equilibrium.
Overall, no differences in the post-COVID symptoms depending on the IL-6 rs1800796 (Table 2), IL-10 rs1800896 (Table 3), TNF-α rs1800629 (Table 4), and IFITM3 rs12252 (Table 5) genotypes were observed. We only found that the A allele of the TNF-α rs1800629 polymorphism and the G allele of the IFITM3 rs12252 polymorphism were more prevalent in obese individuals (p < 0.01), although these associations were based on a small number of subjects (Table 4 and Table 5).
4. Discussion
There is evidence supporting the role of inflammation in the acute COVID-19 phase [4,5] and also in the post-COVID phase [20]. Thus, several polymorphisms associated with inflammation have been related to severe COVID-19 illness in previous studies [7,8,9,10]. Our study did not find an association between four SNPs associated with severe COVID-19, e.g., IL-6 rs1800796, IL-10 rs1800896, TNF-α rs1800629, and IFITM3 rs12252, and the presence of long-lasting post-COVID symptoms more than one year after infection.
We found that almost 90% of our sample of COVID-19 survivors exhibited at least one post-COVID symptom up to 18 months after discharge. Our prevalence rate is much higher than some meta-analyses reporting that 25–30% of COVID-19 survivors exhibit post-COVID symptoms one year after infection [15,16,18]. There are several potential explanations for the observed prevalence rate of post-COVID symptoms in our study. Firstly, the sample included patients who were infected during the initial wave of the pandemic. During this period, the historical SARS-CoV-2 strain was the predominant variant and known as the most aggressive. It has been observed that the prevalence of post-COVID symptoms tends to be higher in patients infected with the historical strain compared to those infected with later variants of concern, such as Alpha, Beta, Delta, or Omicron [25,26]. Secondly, all the participants in this study were infected and developed post-COVID symptoms before being vaccinated. The current evidence suggests that vaccination can decrease the risk of developing post-COVID symptoms if administered before infection, but its effects in patients with ongoing post-COVID symptomatology is unclear [27]. Third, our study included a cohort of hospitalized COVID-19 survivors and hence with moderate to severe COVID-19 illness. Although both hospitalized and non-hospitalized patients can develop post-COVID symptoms, hospitalized patients seem to exhibit a higher risk of some post-COVID symptoms, e.g., dyspnea, pain, and hair loss, than non-hospitalized patients [28]. Thus, we also observed that fatigue, pain, and memory loss were the most prevalent post-COVID symptoms, in agreement with previous meta-analyses [29,30,31].
The underlying mechanisms explaining the development of post-COVID symptoms are not fully understood, and different mechanisms are proposed: viral persistence, long-lasting inflammation, immune system dysregulation, autoimmunity, the reactivation of latent infections, endothelial dysfunction, and alteration in the gut microbiota [32]. Our study did not find an association between the four SNPs associated with inflammation and the development of post-COVID symptoms. The current results agree with a previous study showing that other polymorphisms associated with SARS-CoV-2 trophism, e.g., ACE2 rs2285666, ACE2 rs2074192, TMPRSS2 rs12329760, and TMPRSS2 rs2070788, did not predispose patients to developing post-COVID symptoms either [33]. The lack of a potential influence of inflammatory SNPs on post-COVID symptoms does not exclude the role of the products (inflammatory biomarkers levels) regulated by these polymorphisms. In fact, long-lasting systemic inflammation after the acute COVID-19 phase has been associated with a higher number of post-COVID symptoms [20]; however, it seems that the inflammatory biomarker levels are highly fluctuating [21,22]. Thus, it has been speculated that specific genes could influence particular post-COVID symptoms, although this hypothesis has still not been investigated. Finally, it is also possible that multiple genetic variants potentially modulate the inflammatory response [34].
Finally, the results of the current study should be considered according to its potential limitations. First, the sample consisted of previously hospitalized COVID-19 survivors; therefore, the role of the investigated polymorphisms in non-hospitalized patients should not be extrapolated. Thus, the cohort of this study consisted of patients infected during the first wave of the COVID-19 pandemic, when the historical SARS-CoV-2 variant was predominant. It remains unclear whether the investigated SNPs are associated with post-COVID symptoms in individuals infected with other SARS-CoV-2 variants of concern, although this seems unlikely. Second, the data were self-reported and collected longer than one year after hospitalization. Although we specifically asked for symptoms starting no later than one month after the infection, we cannot exclusively attribute to SARS-CoV-2 infection their development. Additionally, the present study focused solely on four polymorphisms commonly linked to COVID-19 severity and inflammation. At present, it is unknown whether analyses of different SNPs might produce different outcomes. Population-based studies that include whole-genome analysis could be instrumental in identifying additional genes associated with post-COVID symptoms.
5. Conclusions
This study showed that four polymorphisms associated with inflammation and severe COVID-19, e.g., IL-6 rs1800796, IL-10 rs1800896, TNF-α rs1800629, and IFITM3 rs12252, did not cause predisposition to developing post-COVID symptomatology in a cohort of previously hospitalized COVID-19 survivors infected during the first wave of the pandemic.
Author Contributions
All the authors cited in the manuscript made substantial contributions to the concept, design, and execution of the work; the analysis and interpretation of the data; and drafting or revising the manuscript and have read and approved the final version of the paper. Conceptualization, all authors; methodology, C.F.-d.-l.-P., G.D.-G.; A.G.-C. and S.M.G.-S., software, S.A.-Q.; validation, all authors; formal analysis, J.T.-M., G.D.-G., A.G.-C., S.M.G.-S. and O.J.P.-V.; investigation, all authors; resources, J.T.-M., P.R.-M., A.I.F.-M. and L.A.-N.; writing—original draft preparation, all authors; writing—review and editing, all authors; visualization, all authors; supervision, L.A.-N. and R.G.; project administration, L.A.-N.; funding acquisition, C.F.-d.-l.-P. and L.A.-N. All authors have read and agreed to the published version of the manuscript.
Funding
The project was supported by a grant from Novo Nordisk Foundation NNF21OC0067235 (Denmark) and by a grant associated with the Fondo Europeo De Desarrollo Regional—Recursos REACT-UE del Programa Operativo de Madrid 2014–2020, en la línea de actuación de proyectos de I+D+i en materia de respuesta a COVID 19 (LONG-COVID-EXP-CM). Neither sponsor had a role in the design, collection, management, analysis, or interpretation of the data or draft, review, or approval of the manuscript or its content. The authors were responsible for the decision to submit the manuscript for publication, and the sponsors did not participate in this decision.
Institutional Review Board Statement
The study was conducted in accordance with the Declaration of Helsinki and was approved by the Institutional Ethics Committees of all institutions/hospitals involved (URJC0907202015920; HCSC20/495E, HSO25112020; HUFA 20/126; HUIL/092-20).
Informed Consent Statement
Informed consent was obtained from all subjects involved in the study.
Data Availability Statement
All data derived from this study are presented in the text.
Acknowledgments
The Center for Neuroplasticity and Pain (CNAP) is supported by the Danish National Research Foundation (DNRF121) and Novo Nordisk Foundation (NNF21OC0067235). We also thank the Genomics Unit, Madrid Science Park Foundation, Spain, for its valuable support.
Conflicts of Interest
The authors declare no conflicts of interest.
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Table 1.
Pre-infection data and post-COVID symptoms of the total sample.
| Total Sample (n = 408) | |
|---|---|
| Age, mean (SD), years | 58.5 (14.0) |
| Sex, female n (%) | 198 (48.5%) |
| Weight, mean (SD), kg. | 80.1 (17.0) |
| Height, mean (SD), cm. | 166.5 (9.5) |
| Number of co-morbidities, mean (SD) | 1.2 (1.0) |
| Medical co-morbidities, n (%) | |
| Hypertension | 143 (35.0%) |
| Obesity | 98 (24.0%) |
| Diabetes | 43 (10.5%) |
| Asthma | 38 (9.3%) |
| Cardiovascular Diseases | 38 (9.3%) |
| Chronic Obstructive Pulmonary Disease | 10 (2.5%) |
| Rheumatological Diseases | 3 (0.7%) |
| Number of post-COVID symptoms, mean (SD) | 3.0 (1.7) |
| Post-COVID symptoms, n (%) | |
| Fatigue | 283 (69.3%) |
| Pain Symptoms | 167 (40.9%) |
| Memory Loss | 111 (27.2%) |
| Hair Loss | 105 (25.7%) |
| Concentration Loss | 47 (11.5%) |
| Cognitive Blunting—Brain Fog | 45 (11.0%) |
| Dyspnoea | 80 (19.6%) |
| Ocular Disorders | 45 (11.0%) |
| Skin Rashes | 56 (13.7%) |
| Anosmia | 39 (9.5%) |
| Gastrointestinal Disorders | 29 (7.1%) |
| Ageusia | 23 (5.6%) |
| Days in hospital, mean (SD) | 8.2 (7.8) |
Table 2.
Pre-infection data and post-COVID symptoms according to the IL-6 rs1800796 polymorphism.
| G/G (n = 322) | C/G (n = 78) | C/C (n = 8) | p-Value | |
|---|---|---|---|---|
| Age, mean (SD), years | 58.7 (14.0) | 58.5 (14.5) | 57.0 (14.5) | 0.935 |
| Sex, female n (%) | 158 (49.1%) | 35 (44.9%) | 5 (62.5%) | 0.757 |
| Weight, mean (SD), kg. | 80.1 (16.7) | 79.7 (17.7) | 76.2 (20.4) | 0.806 |
| Height, mean (SD), cm. | 166.5 (10.0) | 167 (8.8) | 163 (8.8) | 0.577 |
| Number of co-morbidities, mean (SD) | 1.2 (0.95) | 1.3 (1.0) | 0.75 (0.7) | 0.310 |
| Medical co-morbidities, n (%) | ||||
| Hypertension | 110 (34.1%) | 31 (39.7%) | 2 (25.0%) | 0.672 |
| Obesity | 78 (24.2%) | 19 (24.4%) | 1 (12.5%) | 0.798 |
| Diabetes | 30 (9.3%) | 13 (16.7%) | 0 (0.0%) | 0.131 |
| Asthma | 28 (8.7%) | 10 (12.8%) | 0 (0.0%) | 0.385 |
| Cardiovascular Diseases | 30 (9.3%) | 8 (10.25%) | 0 (0.0%) | 0.663 |
| Chronic Obstructive Pulmonary Disease | 10 (3.1%) | 0 (0.0%) | 0 (0.0%) | 0.263 |
| Rheumatological Diseases | 3 (0.9%) | 0 (0.0%) | 0 (0.0%) | 0.669 |
| Number of post-COVID symptoms, mean (SD) | 3.1 (1.7) | 2.7 (1.7) | 3.0 (1.8) | 0.195 |
| Post-COVID symptoms, n (%) | ||||
| Fatigue | 228 (70.8%) | 49 (62.8%) | 6 (75.0%) | 0.735 |
| Pain Symptoms | 135 (41.9%) | 29 (37.2%) | 3 (37.5%) | 0.981 |
| Memory Loss | 89 (27.6%) | 21 (26.9%) | 1 (12.5%) | 0.783 |
| Hair Loss | 86 (26.7%) | 17 (21.8%) | 2 (25.0%) | 0.985 |
| Concentration Loss | 37 (11.5%) | 10 (12.8%) | 0 (0.0%) | 0.595 |
| Cognitive Blunting—Brain Fog | 38 (11.8%) | 7 (9.0%) | 0 (0.0%) | 0.507 |
| Dyspnoea | 69 (21.4%) | 10 (12.8%) | 1 (12.5%) | 0.275 |
| Ocular Disorders | 37 (11.5%) | 6 (7.7%) | 2 (25.0%) | 0.322 |
| Anosmia | 30 (9.3%) | 8 (10.25%) | 1 (12.5%) | 0.936 |
| Skin Rashes | 41 (12.7%) | 12 (15.4%) | 3 (37.5%) | 0.159 |
| Gastrointestinal Disorders | 22 (6.8%) | 6 (7.7%) | 1 (12.5%) | 0.819 |
| Ageusia | 14 (4.3%) | 8 (10.25%) | 1 (12.5%) | 0.102 |
| Days in hospital, mean (SD) | 8.3 (8.2) | 7.1 (4.9) | 7.0 (6.3) | 0.422 |
Table 3.
Pre-infection data and post-COVID symptoms according to the IL-10 rs1800896 polymorphism.
| T/T (n = 163) | T/C (n = 183) | C/C (n = 62) | p-Value | |
|---|---|---|---|---|
| Age, mean (SD), years | 58.2 (14.2) | 59.5 (13.9) | 57.5 (13.5) | 0.506 |
| Sex, female n (%) | 82 (50.3%) | 93 (50.8%) | 23 (37.1%) | 0.372 |
| Weight, mean (SD), kg. | 81.5 (19.5) | 78.5 (14.3) | 80.5 (16.7) | 0.225 |
| Height, mean (SD), cm. | 167 (9.5) | 165.5 (9.5) | 169 (10.0) | 0.105 |
| Number of co-morbidities, mean (SD) | 1.2 (1.0) | 1.3 (0.9) | 1.0 (1.0) | 0.160 |
| Medical co-morbidities, n (%) | ||||
| Hypertension | 60 (36.8%) | 66 (36.1%) | 17 (27.4%) | 0.541 |
| Obesity | 41 (25.1%) | 45 (24.6%) | 12 (19.3%) | 0.714 |
| Diabetes | 17 (10.4%) | 21 (11.5%) | 5 (8.1%) | 0.773 |
| Asthma | 17 (10.4%) | 17 (9.3%) | 4 (6.4%) | 0.683 |
| Cardiovascular Diseases | 13 (8.0%) | 18 (9.8%) | 7 (11.3%) | 0.730 |
| Chronic Obstructive Pulmonary Disease | 7 (4.3%) | 2 (1.1%) | 1 (1.6%) | 0.149 |
| Rheumatological Diseases | 0 (0.0%) | 3 (1.6%) | 0 (0.0%) | 0.158 |
| Number of post-COVID symptoms, mean (SD) | 3.0 (1.6) | 2.9 (1.7) | 2.9 (1.9) | 0.481 |
| Post-COVID symptoms, n (%) | ||||
| Fatigue | 116 (71.2%) | 123(67.2%) | 44 (71.0%) | 0.895 |
| Pain Symptoms | 70 (42.9%) | 74 (40.4%) | 24 (38.7%) | 0.895 |
| Memory Loss | 42 (25.8%) | 51 (27.9%) | 19 (30.4%) | 0.814 |
| Hair Loss | 39 (23.9%) | 51 (27.9%) | 15 (24.2%) | 0.742 |
| Concentration Loss | 18 (11.05%) | 19 (10.4%) | 10 (16.1%) | 0.501 |
| Cognitive Blunting—Brain Fog | 10 (11.7%) | 21 (11.5%) | 5 (8.05%) | 0.745 |
| Dyspnoea | 39 (23.9%) | 27 (14.7%) | 14 (22.6%) | 0.134 |
| Ocular Disorders | 21 (12.9%) | 17 (9.3%) | 7 (11.3%) | 0.602 |
| Anosmia | 12 (7.4%) | 20 (10.9%) | 7 (11.3%) | 0.502 |
| Skin Rashes | 25 (15.3%) | 26 (14.2%) | 5 (8.05%) | 0.409 |
| Gastrointestinal Disorders | 10 (6.1%) | 14 (7.6%) | 5 (8.05%) | 0.831 |
| Ageusia | 6 (3.7%) | 11 (6.0%) | 6 (9.7%) | 0.229 |
| Days in hospital, mean (SD) | 7.8 (6.0) | 8.3 (9.1) | 8.0 (7.2) | 0.793 |
Table 4.
Pre-infection data and post-COVID symptoms according to the TNF-α rs1800629 polymorphism.
| G/G (n = 324) | A/G (n = 78) | A/A (n = 6) | p-Value | |
|---|---|---|---|---|
| Age, mean (SD), years | 58.4 (14.0) | 60.0 (14.3) | 55.7 (6.5) | 0.580 |
| Sex, female n (%) | 153 (47.2%) | 43 (55.1%) | 2 (33.3%) | 0.577 |
| Weight, mean (SD), kg. | 79.5 (16.5) | 80.0 (18.0) | 101.2 (12.2) | 0.008 |
| Height, mean (SD), cm. | 166.5 (9.5) | 166 (9.5) | 177.5 (14.7) | 0.02 |
| Number of co-morbidities, mean (SD) | 1.25 (1.0) | 1.1 (1.0) | 1.5 (0.85) | 0.403 |
| Medical co-morbidities, n (%) | ||||
| Hypertension | 114 (35.1%) | 28 (35.9%) | 1 (16.7%) | 0.742 |
| Obesity | 78 (24.1%) | 15 (19.25%) | 5 (83.3%) | 0.008 |
| Diabetes | 35 (10.8%) | 7 (9.0%) | 1 (16.7%) | 0.812 |
| Asthma | 32 (9.9%) | 5 (6.4%) | 1 (16.7%) | 0.558 |
| Cardiovascular Diseases | 30 (9.25%) | 8 (10.25%) | 0 (0.0%) | 0.728 |
| Chronic Obstructive Pulmonary Disease | 9 (2.8%) | 1 (1.3%) | 0 (0.0%) | 0.696 |
| Rheumatological Diseases | 2 (0.65%) | 1 (1.3%) | 0 (0.0%) | 0.809 |
| Number of post-COVID symptoms, mean (SD) | 3.0 (1.65) | 2.9 (1.8) | 3.8 (2.4) | 0.324 |
| Post-COVID symptoms, n (%) | ||||
| Fatigue | 228 (70.4%) | 50 (64.1%) | 5 (83.3%) | 0.768 |
| Pain Symptoms | 136 (41.9%) | 28 (35.8%) | 2 (33.3%) | 0.819 |
| Memory Loss | 88 (27.2%) | 22 (28.2%) | 2 (33.3%) | 0.950 |
| Hair Loss | 81 (25.0%) | 23 (29.5%) | 1 (16.7%) | 0.709 |
| Concentration Loss | 36 (11.1%) | 8 (10.25%) | 3 (50.0%) | 0.509 |
| Cognitive Blunting—Brain Fog | 39 (12.1%) | 4 (5.1%) | 2 (33.3%) | 0.065 |
| Dyspnoea | 60 (18.5%) | 19 (24.35%) | 1 (16.7%) | 0.571 |
| Ocular Disorders | 36 (11.1%) | 7 (9.0%) | 2 (33.3%) | 0.224 |
| Anosmia | 34 (10.5%) | 5 (6.4%) | 0 (0.0%) | 0.432 |
| Skin Rashes | 48 (14.8%) | 8 (10.25%) | 0 (0.0%) | 0.409 |
| Gastrointestinal Disorders | 20 (6.2%) | 8 (10.25%) | 1 (16.7%) | 0.323 |
| Ageusia | 21 (6.5%) | 2 (2.5%) | 0 (0.0%) | 0.358 |
| Days in hospital, mean (SD) | 8.25 (8.0) | 7.4 (6.3) | 6.2 (4.0) | 0.554 |
Table 5.
Pre-infection data and post-COVID symptoms according to the IFITM3 rs12252 polymorphism.
| A/A (n = 345) | A/G (n = 58) | G/G (n = 5) | p-Value | |
|---|---|---|---|---|
| Age, mean (SD), years | 59.7 (13.7) | 53.5 (14.8) | 48.6 (11.9) | 0.002 |
| Sex, female n (%) | 161 (46.7%) | 33 (56.9%) | 4 (80.0%) | 0.349 |
| Weight, mean (SD), kg. | 79.5 (17.0) | 80.6 (15.7) | 96.8 (25.9) | 0.07 |
| Height, mean (SD), cm. | 167 (9.5) | 166 (10.0) | 165.5 (9.5) | 0.202 |
| Number of co-morbidities, mean (SD) | 1.2 (0.9) | 1.2 (1.0) | 2.0 (1.2) | 0.168 |
| Medical co-morbidities, n (%) | ||||
| Hypertension | 124 (35.9%) | 16 (27.6%) | 3 (60.0%) | 0.389 |
| Obesity | 73 (21.2%) | 21 (36.2%) | 4 (80.0%) | 0.003 |
| Diabetes | 38 (11.0%) | 5 (5.8%) | 0 (0.0%) | 0.669 |
| Asthma | 33 (9.6%) | 5 (5.8%) | 0 (0.0%) | 0.771 |
| Cardiovascular Diseases | 33 (9.6%) | 5 (5.8%) | 0 (0.0%) | 0.771 |
| Chronic Obstructive Pulmonary Disease | 9 (2.6%) | 1 (1.7%) | 0 (0.0%) | 0.868 |
| Rheumatological Diseases | 1 (0.3%) | 2 (3.45%) | 0 (0.0%) | 0.338 |
| Number of post-COVID symptoms, mean (SD) | 2.9 (1.7) | 3.4 (1.7) | 3.2 (1.9) | 0.204 |
| Post-COVID symptoms, n (%) | ||||
| Fatigue | 234(67.8%) | 46 (79.3%) | 3 (60.0%) | 0.605 |
| Pain Symptoms | 138 (40.0%) | 27 (46.5%) | 2 (40.0%) | 0.540 |
| Memory Loss | 94 (27.2%) | 16 (27.6%) | 2 (40.0%) | 0.863 |
| Hair Loss | 88 (25.5%) | 14 (24.1%) | 3 (60.0%) | 0.309 |
| Concentration Loss | 41 (11.9%) | 6 (10.35%) | 0 (0.0%) | 0.709 |
| Cognitive Blunting—Brain Fog | 39 (11.3%) | 6 (10.35%) | 0 (0.0%) | 0.740 |
| Dyspnoea | 60 (17.4%) | 19 (32.8%) | 3 (60.0%) | 0.04 |
| Ocular Disorders | 38 (11.0%) | 6 (10.35%) | 1 (20.0%) | 0.823 |
| Anosmia | 31 (9.9%) | 8 (13.8%) | 0 (0.0%) | 0.430 |
| Skin Rashes | 47 (13.6%) | 7 (12.1%) | 2 (40.0%) | 0.268 |
| Gastrointestinal Disorders | 27 (7.8%) | 2 (3.5%) | 0 (0.0%) | 0.427 |
| Ageusia | 17 (4.9%) | 6 (10.35%) | 0 (0.0%) | 0.238 |
| Days in hospital, mean (SD) | 8.0 (7.7) | 8.4 (7.4) | 8.2 (8.7) | 0.941 |
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Fernández-de-las-Peñas, C.; Díaz-Gil, G.; Gil-Crujera, A.; Gómez-Sánchez, S.M.; Ambite-Quesada, S.; Torres-Macho, J.; Ryan-Murua, P.; Franco-Moreno, A.I.; Pellicer-Valero, O.J.; Arendt-Nielsen, L.; et al. Inflammatory Polymorphisms (IL-6 rs1800796, IL-10 rs1800896, TNF-α rs1800629, and IFITM3 rs12252) Are Not Associated with Post-COVID Symptoms in Previously Hospitalized COVID-19 Survivors. Viruses 2024, 16, 275. https://doi.org/10.3390/v16020275
AMA Style
Fernández-de-las-Peñas C, Díaz-Gil G, Gil-Crujera A, Gómez-Sánchez SM, Ambite-Quesada S, Torres-Macho J, Ryan-Murua P, Franco-Moreno AI, Pellicer-Valero OJ, Arendt-Nielsen L, et al. Inflammatory Polymorphisms (IL-6 rs1800796, IL-10 rs1800896, TNF-α rs1800629, and IFITM3 rs12252) Are Not Associated with Post-COVID Symptoms in Previously Hospitalized COVID-19 Survivors. Viruses. 2024; 16(2):275. https://doi.org/10.3390/v16020275
Chicago/Turabian StyleFernández-de-las-Peñas, César, Gema Díaz-Gil, Antonio Gil-Crujera, Stella M. Gómez-Sánchez, Silvia Ambite-Quesada, Juan Torres-Macho, Pablo Ryan-Murua, Ana I. Franco-Moreno, Oscar J. Pellicer-Valero, Lars Arendt-Nielsen, and et al. 2024. "Inflammatory Polymorphisms (IL-6 rs1800796, IL-10 rs1800896, TNF-α rs1800629, and IFITM3 rs12252) Are Not Associated with Post-COVID Symptoms in Previously Hospitalized COVID-19 Survivors" Viruses 16, no. 2: 275. https://doi.org/10.3390/v16020275
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