Advertisement
Browse Subject Areas
?

Click through the PLOS taxonomy to find articles in your field.

For more information about PLOS Subject Areas, click here.

  • Loading metrics

Open Access

Peer-reviewed

Research Article

Association of G-Protein-Coupled Receptors autoantibodies with vasoregulation in Post-COVID

Abstract

Background

The Post-COVID syndrome is associated with the generation of autoantibodies to vasoregulative G-protein coupled receptors (GPCR). It remains elusive, however, whether these autoantibodies play a pathophysiological role in this disease. The present study investigates whether detection and concentration of GPCR autoantibodies are related to vascular function in patients with Post-COVID.

Materials and methods

We performed a cross-sectional study, enrolling 80 patients with Post-COVID and 54 individuals with a history of SARS-CoV-2 infection without persisting symptoms (control group). ELISA measurement of GPCR autoantibodies encompassed autoantibodies to Angiotensin-II-Receptor-1 (AGTR2), Beta-1 Adrenergic Receptor (ADRB1), Beta-2 Adrenergic Receptor (ADRB2), Endothelin Receptor (EDNRA), Muscarinergic Choline Receptor 3 (CHRM3), and Muscarinergic Choline Receptor 4 (CHRM4). Endothelium-dependent vasodilation was assessed by flow mediated dilation (FMD). Measurement of central aortic blood pressure and capillary nailfold capillary microscopy were performed as additional assessments of vasoregulatory function. Lipoprotein-associated phospholipase A2 (Lp-PLA2) served as markers of vascular inflammation.

Results

52 (65%) patients with Post-COVID had positive autoantibody findings above previously established cut-off values, the incidence was lower in the non-Post-COVID group (n = 12, 22.2%, p = 0.0001). The median concentrations for AGTR2, ADRB1, CHRM3 and CHRM4 autoantibodies were significantly higher in the symptomatic cohort (p < 0.05 each). Spearman correlation analysis showed a strong and significant negative correlation of several GPCR autoantibodies with aortic systolic blood pressure (AGTR2 p = 0.026, ADRB1 p = 0.001, ADRB2 p = 0.012) and aortic diastolic blood pressure (ADRB1 p = 0.005, CHRM4 p = 0.046) in Post-COVID. High EDNRA autoantibodies titers were associated with FMD (p = 0.038). There was no significant association of any GPCR autoantibody concentration with FMD or Lp-PLA2 in the control group.

Conclusion

GPCR autoantibodies were highly prevalent in this Post-COVID cohort. Several GPCR autoantibodies were associated with measures of vasorelaxation like lower systolic and diastolic aortic blood pressure and stronger endothelium-dependent vasodilation. However, given the absence of differences in microvascular and macrovascular function, the precise role of GPCR autoantibodies remains elusive.

Citation: Seibert FS, Kurucay M, Wiemers L, Stervbo U, Sander O, Segelbacher M, et al. (2026) Association of G-Protein-Coupled Receptors autoantibodies with vasoregulation in Post-COVID. PLoS One 21(2): e0343264. https://doi.org/10.1371/journal.pone.0343264

Editor: Eliseo A. Eugenin, University of Texas Medical Branch at Galveston, UNITED STATES OF AMERICA

Received: February 11, 2025; Accepted: February 3, 2026; Published: February 24, 2026

Copyright: © 2026 Seibert et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

Data Availability: The dataset is publicly available and can be accessed at the following DOI: https://doi.org/10.6084/m9.figshare.30127723.

Funding: The author(s) received no specific funding for this work.

Competing interests: The authors have declared that no competing interests exist.

Introduction

In contrast to a decreasing number of severe acute courses of COVID-19, the incidence of Post-COVID remains at a high level, going along with a significant socioeconomic impact. About 5% of all SARS-CoV-2-infected patients do not completely recover from COVID-19 and fulfill the criteria of Post-COVID [13]. The Post-COVID syndrome is defined by the WHO as the continuation or the development of not otherwise explainable new symptoms after the onset of an acute SARS-CoV-2-infection for a duration of at least two months. Post-COVID presents with a variety of multiorgan disorders, including fatigue, post exertional malaise, shortness of breath, myalgia and cognitive impairment. Post-COVID shows striking similarities with the encephalomyelitis/chronic fatigue syndrome (ME/CFS) and is increasingly recognized as a SARS-CoV-2 related ME/CFS variant [4].

The pathophysiology of both of the above-mentioned diseases is incompletely understood and currently under investigation. Postinfectious persisting tissue damage, autoimmunity, vascular dysfunction and virus persistence are four prominent hypotheses in this context [5]. We recently linked the generation of autoantibodies against vasoregulatory G-protein coupled receptors (GPCR) to the intensity of neurological disorders including psychomotor speed, visual search, attention, and fatigue [6].

The hypothesis of impaired micro- and macrovascular dysregulation following SARS-CoV-2 infection, results from a sound body of evidence [7]. The underlying mechanisms, however, remain elusive. The present study investigates whether the generation of autoantibodies to GPCR is associated with alterations in vasoregulatory function.

Materials and methods

Protocol and patients

We performed a monocentric cross-sectional study at the University Hospital of the Ruhr-University Bochum, Germany, enrolling 80 patients with Post-COVID. Post-COVID was diagnosed according to the German S1 guideline [8]. All neuropsychological assessments were performed applying to the German version of the “Consortium to Establish a Registry for Alzheimer’s Disease Neuropsychological Assessment Battery” [9]. Enrollment encompassed mild to moderate SARS-CoV-2 infection up to 12 months prior to inclusion. A second group (n = 54) of individuals had SARS-CoV-2 infection, but without presenting ongoing symptoms (control group). All patients signed informed consent. The Ethics Committee of the Ruhr-University of Bochum approved the study (ID 22–7491) in accordance with the 1964 Declaration of Helsinki and its later amendments.

Measurement of autoantibodies to GPCR

The GPCR autoantibody panel was selected based on prior biological relevance and established use in the literature. We applied a commercially available GPCR autoantibody panel that has been used in our previous work [6]. GPCR autoantibodies encompassed autoantibodies against Angiotensin-II-Receptor-1 (AGTR2), Beta-1 Adrenergic Receptor (ADRB1), Beta-2 Adrenergic Receptor (ADRB2), Endothelin Receptor (EDNRA), Muscarinergic Choline Receptor 3 (CHRM3), and Muscarinergic Choline Receptor 4 (CHRM4), all measured by ELISA. Serum was collected in a S-Monovette Serum collection tube (Sarstedt, Germany) and processed per manufacturer’s instructions. Purified serum was stored at −20°C until use. ELISA systems for detection of autoantibodies against AGTR2, ADRB1, ADRB2, EDNRA, CHRM3, and CHRM4 were all obtained from CellTrend, Germany. Autoantibodies in serum were determined per manufacturer’s instructions and normalized using the provided standard. Cut-offs for the detection have been chosen according to the manufacturer. The following cut-offs were used to define presence of autoantibodies: AGTR2: > 10 U/ml; ADRB1: > 15 U/ml; ADRB2: > 8 U/ml; EDNRA: > 10 U/ml; CHRM3: > 10 U/ml; CHRM4: > 6 U/ml.

Measurement of markers of vascular and systemic inflammation

Vascular inflammation was assessed by measurement of lipoprotein-associated phospholipase A2 (Lp-PLA2). Lp-PLA2 is regarded as a marker of vascular inflammation [10]. Moreover, Lp-PLA2 has been found to be correlated with several comorbidities, complications and the severity of COVID-19 [11]. Both parameters were assessed according to the manufacturer’s protocol (kit number L26722 [Asbach Medical] and 09877 [Roche], respectively)

Measurement of endothelium-dependent vasodilation by flow-mediated dilation

Endothelium-dependent vasodilation was assessed by flow mediated dilation (FMD). Vascular endothelial function of the right brachial artery was studied with ultrasonography (Aloka/Hitachi, Prosound alpha 6) with a high-frequency (5–13 MHz) linear-array transducer. The examinations were performed under standard conditions (room temperature 22 °C, quiet environment). Blood pressure was measured by an oscillometric method before initiation of FMD measurement. Participants were positioned in a supine position for 15 min to avoid a potential effect of stress and they were instructed not to speak during the examination. Assessment of endothelium-dependent vasodilation was done at the level of right brachial artery 5–10 cm above the antecubital fossa, according to the recommendations for FMD assessment [12,13].

The tracking gate followed the motion of the vessel walls caused by pulsations and automatically measured the change in vessel diameter with a precision up to 0.01 mm in real time. The waveform of diameter changes over the cardiac cycle was displayed in real time using the FMD-mode of the eTRACKING system. The internal diameter of right brachial artery was continuously monitored using following protocol: 1 min recording of baseline diameter at rest, 5 min recording during a forearm ischemia induced by inflation of a pneumatic forearm cuff 50 mmHg above systolic blood pressure, and 3 min of post-deflation diameter recording. All the examinations were performed by one and the same specialist trained in 2D and Doppler ultrasonography. To minimize operator-dependent error, a mechanical probe holder was used with the fixed angle approximately 60° between the probe and the vessel orientation in all the examinations.

Central aortic blood pressure

We performed a non-invasive pulse wave analysis to investigate central aortic blood pressure. The Mobil-O-Graph device performs an oscillometric assessment of peripheral blood pressure and uses tonometric contour analysis of the brachial arterial pulse wave in order to provide systolic, diastolic and mean blood pressure values after a stepwise deflation process of the cuff. Calibration is performed using systolic and diastolic pressure. This system calculates central blood pressure, aortic PWV and additional central hemodynamic indices, all based on the oscillometric recording of pulse waves at the brachial artery site. In a first step, the recorded pulse waves are checked for their plausibility and qualified according to pre-defined quality criteria. Once the input signal has qualified as acceptable, the concepts of wave harmonics and Fourier analysis are applied for the calculation of an aortic pressure curve. The device has been validated by a comparison to intraarterial measurements [14,15] and an established tonometric method [16,17]. Central blood pressure measurement was not available in the control group.

Nailfold capillary microscopy

Standardized capillary microscopic examinations of the nailfolds of both hands (digits II-V) were performed on patients diagnosed with Post-COVID. The images (close-up with details representing 1 mm/210-fold magnification for each patient) were pseudonymized and stored. The images were assessed according to standardized criteria with regard to capillary density and morphological changes including vessel diameter variability, as well as elongation and ramification (neoangiogenesis). The lower cut-off for normal density was 7/mm. Nailford capillary microscopy was not performed in the control group.

Statistics

Data were analyzed for Gaussian distribution (D’Agostino Pearson). In case of normal distribution, data are presented as mean with standard deviation (SD), otherwise, data are given as median with interquartile range (IQR). Differences between groups were assessed using the Mann-Whitney-U-test. If relevant, Spearman correlation was performed.

Results

Patient demographics of both cohorts are summarized in Table 1. With 45 years, both groups were of similar age. Sex distribution analysis revealed that significantly more women were affected in the Post-COVID cohort (72.5%, p = 0.0022). BMI was lower for participants without Post-COVID (24.9 ± 3.34 vs. 27.6 ± 5.9, p = 0.0214). In our cohort, 40 out of 80 patients with Post-COVID (50%) had received at least one SARS-CoV-2 vaccination prior to study inclusion, whereas 48 out of 54 individuals (88.9%) in the non-Post-COVID group were vaccinated, resulting in the reported significant difference (p = 0.0001; Table 1). Accordingly, 40 patients (50%) in the Post-COVID group and 6 subjects (11.1%) in the control group were unvaccinated. Neurological impairment as assessed via CERAD-Plus was numerically stronger in the Post-COVID group, but without reaching statistical significance (p = 0.1061). Prevalence of cardiovascular comorbidities like diabetes, coronary heart disease, hypercholesterinemia, hypertension and smoking did not significantly differ between the groups. 52 (65%) patients with Post-COVID had positive GPCR autoantibody findings above previously established cut-off values. The median absolute concentrations and the subgroup of patients, presenting at least one positive GPCR autoantibody, are presented in Table 2.

thumbnail
Download:
Table 1. Population characteristics.

https://doi.org/10.1371/journal.pone.0343264.t001

thumbnail
Download:
Table 2. GPCR autoantibody findings and FMD in Post-COVID and no Post-COVID.

https://doi.org/10.1371/journal.pone.0343264.t002

Amongst 54 patients without Post-COVID, a significantly lower amount (n = 12, 22.2%, p = 0.001) were positive for at least one GPCR autoantibody. As seen in Table 2, the median concentrations for AGTR2, ADRB1, CHRM3 and CHRM4 autoantibodies were significantly lower in the asymptomatic cohort (p < 0.05 each). No correlation for any GPCR autoantibodies and FMD was seen in patients without Post-COVID (p > 0.05 each, Table 3).

thumbnail
Download:
Table 3. Spearman correlation analysis for hemodynamic parameters and nailfold capillaroscopy.

https://doi.org/10.1371/journal.pone.0343264.t003

In order to elucidate the relationship between the GPCR autoantibodies in Post-COVID and the vascular function, we compared any difference in vasodilatory capacity between groups. Given the numerical trend toward lower FMD values in Post-COVID (Table 2), we subsequently performed a Spearman correlation analysis between the autoantibody concentrations and FMD. EDNRA concentrations were positively associated with FMD (p = 0.0382) in patients with Post-COVID. However, this association did not remain statistically significant after adjustment for covariates including sex, BMI, and vaccination status (p = 0.0745). Furthermore, there was a negative correlation between AGTR2-, ADRB1-, and ADRB1-autoantibodies with central systolic blood pressure (p = 0.0276, p = 0.0027, p = 0.0013, respectively) and a significant negative association between central diastolic blood pressure and anti-ADRB1 and -CHMR4-concentrations (ADRB1 p = 0.0045, CHRM4 p = 0.0086) in patients suffering from Post-COVID. Fig 1 illustrates the positive association of EDNRA and FMD in Post-COVID, Fig 2 the significant associations of GPCR autoantibodies with systolic and diastolic central aortic blood pressure in Post-COVID.

thumbnail
Download:
Fig 1. Correlation analysis of flow-mediated dilation (FMD) with GPCR autoantibodies in Post-COVID and in the control group.

Concentrations of (A) EDNRA autoantibodies in the Post-COVID population are positively associated with FMD in Spearman correlation, whereas there is no correlation in the no Post-COVID population (B). Asterisks indicate p-value (**** < 0.0001; *** < 0.001, ** < 0.01, * < 0.05).

https://doi.org/10.1371/journal.pone.0343264.g001

thumbnail
Download:
Fig 2. Correlation analysis of aortic systolic and diastolic blood pressure with GPCR autoantibodies in Post-COVID Concentrations of (A) ATGR2, (B) ADRB1 and (C) ADRB2 autoantibodies are inversely associated with central systolic blood pressure. Concentrations of (D) ADRB1 and (E) CHMR4 autoantibodies were inversely associated with central diastolic blood pressure. Asterisk indicate p-value (**** < 0.0001; *** < 0.001, ** < 0.01, * < 0.05). cSYS – central systolic blood pressure; cDIA – central diastolic blood pressure.

https://doi.org/10.1371/journal.pone.0343264.g002

In both groups, none of the GPCR autoantibodies were associated with Lp-PLA2 (p > 0.05). We investigated morphological and functional changes in microcirculation as seen by nailfold capillaroscopy. None of the investigated sub-entities (capillary density, vessel diameter variability, elongation, ramification) had a significant association with GPCR autoantibodies in Post-COVID (p > 0.05 each).

Discussion

“Take Post-COVID condition seriously by urgently investing in research, recovery, and rehabilitation”. The present study aims to follow this urgent call from the World Health Organization, who believes millions will be affected in the years to come [18]. The study’s findings confirm an increased generation of GPCR autoantibodies in Post-COVID compared to subjects without persisting complaints after SARS-CoV-2 infections. Beyond this descriptive finding, it remains unclear why higher autoantibody levels in Post-COVID patients do not translate into overt differences in vascular parameters when compared to Non–Post-COVID individuals.

Preliminary findings suggest that immune and vascular dysregulations may be involved in the pathophysiology of Post-COVID [19]. We and others have shown that Post-COVID is associated with increased prevalence of GPCR autoantibodies. We have recently demonstrated that the concentrations of these autoantibodies correlate with the intensity of cognitive and physical impairment in Post-COVID [6]. A correlation between levels of autoantibodies against immuno- and vasoregulatory GPCR and cardiovascular clinical severity was found in another study of acute COVID-19 [20]. By induction or alteration of signaling, these autoantibodies can regulate the autonomous nervous system, and the function of immune and endothelial cells function – factors known to be involved in COVID-19 pathogenesis [19]. The present study further contributes to our understanding of these autoantibodies: It shows that GPCR autoantibody concentrations might have an association with markers of vasodilation. FMD is a measure of endothelial function, since the dilation of the brachial artery is mediated by NO release of intact endothelial cells after a transient period of ischemia. In line with this finding, autoantibody concentrations inversely correlate with central systolic blood pressure. There is a notably higher level of ADRB2 autoantibodies in the non-Post-COVID group with at least one positive GPCR autoantibody compared to Post-COVID patients, which may point toward a modulatory or compensatory role of these autoantibodies in maintaining vascular and immune homeostasis. Endogenous autoantibodies against GPCRs (including β2-adrenergic receptors) are known to act as functional modulators of receptor signaling and immune regulation rather than just disease markers [21]. There is a growing body of data on the complex nature of these autoantibodies, which are known to exert agonistic and antagonistic effects on the GPCR, consequently exerting both vasoconstrictor and vasodilatory effects [22].

Endothelin-1 receptor type A (EDNRA) is a G-protein-coupled receptor expressed on the surface of a great variety of cells, e.g., immune cells, vascular smooth muscle cells and endothelial cells [2325]. Certain autoantibodies are specific for these receptors and can regulate their function, some yielding vasoconstriction through ETA, but also mediating inflammatory signals [26]. On the other hand, there are vasodilator effects as the result of a release of substances like nitric oxide (NO), prostacyclin and endothelium-derived hyperpolarizing factor (EDHF) through ETB-receptor-stimulation [27]. An improved vascular function, measured by predominant NO-mediated dilation, has been described by an increasing concentration of EDNRA autoantibodies in our Post-COVID cohort and might mirror the mechanism described above. Flow mediated dilation slows down the pulse pressure wave, leading to a reduced central blood pressure, as observed in various studies as well as in this very one [28,29]. All the other GPCR autoantibodies, that have been investigated in this study, are involved in vasoregulation as well via either angiotensin receptors, betaadrenergic or muscarinergic receptors [30,31]. Thus, they are of crucial relevance for local vasomotor tone. It has been hypothesized, that alterations in perfusion might be the pathophysiological basis for Post-COVID symptoms like fatigue or mnestic deficits. At first sight, it might appear surprising, that the present study presents an association of GPCR autoantibody concentrations and vasodilation instead of vasoconstriction. Vasodilation, however, can go along with both local hyperemia and systemic hypotension and can thereby alter physiological conditions as well. Thus, the hypothesis of cerebral vasodilation as the pathophysiological basis of migraine was supported for decades. Noteworthy, however, the present study – due to its descriptive character – is not able to prove a causal relation between GPCR autoantibodies, changes in vasoregulation and Post-COVID symptoms. Ultimately, our data raise the question of how increased autoantibody levels in Post-COVID patients can be reconciled with the absence of measurable functional vascular (FMD) differences between groups. One possible explanation is that autoantibodies may exert harmful or dysregulating effects on the vasculature, but that compensatory mechanisms, such as counterregulatory endothelial or neurohumoral pathways, may mask these effects at the macroscopic level, resulting in preserved FMD and central blood pressure values.

Central aortic blood pressure and FMD are markers of arterial function. The present study investigated capillary function as well by means of nailfold microscopy in the Post-COVID patients. Our findings did not reveal an association between GPCR autoantibody concentrations and capillary function. This also aligns with the hypothysesis, which suggests that autoantibodies might contribute to maintaining vascular homeostasis rather than impairing it. If autoantibodies serve a compensatory or modulatory purpose in Post-COVID patients, they could help preserve vascular parameters within normal ranges, potentially at the expense of other organ systems such as the central nervous system. In this scenario, it would be conceivable that autoantibodies support vascular stability but simultaneously participate in cognitive dysfunction, a hypothesis that warrants explicit consideration in future mechanistic studies.

Microinflammatory processes have been proposed as an alternative pathomechanism in Post-COVID. A recent review investigated inflammatory and vascular biomarkers in Post-COVID. C-reactive protein was found to be increased in COVID-19 survivors, that suffered from Post-COVID [32]. In the present study, we focused on vascular inflammation. Lp-PLA2 concentrations were not associated with GPCR autoantibodies. Our results about nailfold capillaroscopy supports this finding.

A limitation of this study is the limited availability of hemodynamic data in the control group. In addition, the absence of subgroup analyses for potential confounding variables (e.g., COVID-19 severity, vaccination status) also represents a limitation. Therefore, we cannot exclude the possibility that other unmeasured or uncontrolled factors may account for the observed associations. It cannot be ruled out that autoantibodies do not play a functional role in vascular regulation, given that no vascular alterations were observed between Post-COVID and Non–Post-COVID groups. A more rigorous evaluation of vascular parameters alongside autoantibody measurements or a larger sample size would be required to clarify this point.

The present study confirms that Post-COVID is associated with an increased generation of GPCR autoantibodies. It has previously been shown that the concentration of these autoantibodies correlates with neurological symptoms of Post-COVID. Although certain autoantibodies were associated with parameters of vasoregulation, the present data do not provide evidence for a causal, pathogenic, or etiologically relevant role of these autoantibodies in Post-COVID. Future longitudinal and mechanistic studies are required to determine whether GPCR autoantibodies are merely markers of immune dysregulation or actively involved in Post-COVID pathophysiology.

References

  1. 1. Menges D, Ballouz T, Anagnostopoulos A, Aschmann HE, Domenghino A, Fehr JS, et al. Burden of post-COVID-19 syndrome and implications for healthcare service planning: A population-based cohort study. PLoS One. 2021;16(7):e0254523. pmid:34252157
  2. 2. Global Burden of Disease Long COVID Collaborators, Wulf Hanson S, Abbafati C, Aerts JG, Al-Aly Z, Ashbaugh C, et al. Estimated Global Proportions of Individuals With Persistent Fatigue, Cognitive, and Respiratory Symptom Clusters Following Symptomatic COVID-19 in 2020 and 2021. JAMA. 2022;328(16):1604–15. pmid:36215063
  3. 3. Soriano JB, Murthy S, Marshall JC, Relan P, Diaz JV, WHO Clinical Case Definition Working Group on Post-COVID-19 Condition. A clinical case definition of post-COVID-19 condition by a Delphi consensus. Lancet Infect Dis. 2022;22(4):e102–7. pmid:34951953
  4. 4. Kedor C, Freitag H, Meyer-Arndt L, Wittke K, Hanitsch LG, Zoller T, et al. A prospective observational study of post-COVID-19 chronic fatigue syndrome following the first pandemic wave in Germany and biomarkers associated with symptom severity. Nat Commun. 2022;13(1):5104. pmid:36042189
  5. 5. Davis HE, McCorkell L, Vogel JM, Topol EJ. Long COVID: major findings, mechanisms and recommendations. Nat Rev Microbiol. 2023;21(3):133–46. pmid:36639608
  6. 6. Seibert FS, Stervbo U, Wiemers L, Skrzypczyk S, Hogeweg M, Bertram S, et al. Severity of neurological Long-COVID symptoms correlates with increased level of autoantibodies targeting vasoregulatory and autonomic nervous system receptors. Autoimmun Rev. 2023;22(11):103445. pmid:37689093
  7. 7. Teuwen L-A, Geldhof V, Pasut A, Carmeliet P. COVID-19: the vasculature unleashed. Nat Rev Immunol. 2020;20(7):389–91. pmid:32439870
  8. 8. Koczulla AR, Ankermann T, Behrends U, Berlit P, Böing S, Brinkmann F, et al. S1 Guideline Post-COVID/Long-COVID. Pneumologie. 2021;75(11):869–900. pmid:34474488
  9. 9. Schmid NS, Ehrensperger MM, Berres M, Beck IR, Monsch AU. The Extension of the German CERAD Neuropsychological Assessment Battery with Tests Assessing Subcortical, Executive and Frontal Functions Improves Accuracy in Dementia Diagnosis. Dement Geriatr Cogn Dis Extra. 2014;4(2):322–34. pmid:25298776
  10. 10. Rosenson RS, Hurt-Camejo E. Phospholipase A2 enzymes and the risk of atherosclerosis. Eur Heart J. 2012;33(23):2899–909. pmid:22802388
  11. 11. Dua P, Mishra A, Reeta KH. Lp-PLA2 as a biomarker and its possible associations with SARS-CoV-2 infection. Biomark Med. 2022;16(10):821–32. pmid:35694871
  12. 12. Corretti MC, Anderson TJ, Benjamin EJ, Celermajer D, Charbonneau F, Creager MA, et al. Guidelines for the ultrasound assessment of endothelial-dependent flow-mediated vasodilation of the brachial artery: a report of the International Brachial Artery Reactivity Task Force. J Am Coll Cardiol. 2002;39(2):257–65. pmid:11788217
  13. 13. Thijssen DHJ, Black MA, Pyke KE, Padilla J, Atkinson G, Harris RA, et al. Assessment of flow-mediated dilation in humans: a methodological and physiological guideline. Am J Physiol Heart Circ Physiol. 2011;300(1):H2-12. pmid:20952670
  14. 14. Weber T, Wassertheurer S, Rammer M, Maurer E, Hametner B, Mayer CC, et al. Validation of a brachial cuff-based method for estimating central systolic blood pressure. Hypertension. 2011;58(5):825–32. pmid:21911710
  15. 15. Hametner B, Wassertheurer S, Kropf J, Mayer C, Eber B, Weber T. Oscillometric estimation of aortic pulse wave velocity: comparison with intra-aortic catheter measurements. Blood Press Monit. 2013;18(3):173–6. pmid:23571229
  16. 16. Weiss W, Gohlisch C, Harsch-Gladisch C, Tölle M, Zidek W, van der Giet M. Oscillometric estimation of central blood pressure: validation of the Mobil-O-Graph in comparison with the SphygmoCor device. Blood Press Monit. 2012;17(3):128–31. pmid:22561735
  17. 17. Luzardo L, Lujambio I, Sottolano M, da Rosa A, Thijs L, Noboa O, et al. 24-h ambulatory recording of aortic pulse wave velocity and central systolic augmentation: a feasibility study. Hypertens Res. 2012;35(10):980–7. pmid:22622282
  18. 18. World Health Organization. World Health Organization. https://www.who.int/europe
  19. 19. Sotzny F, Filgueiras IS, Kedor C, Freitag H, Wittke K, Bauer S, et al. Dysregulated autoantibodies targeting vaso- and immunoregulatory receptors in Post COVID Syndrome correlate with symptom severity. Front Immunol. 2022;13:981532. pmid:36238301
  20. 20. Cabral-Marques O, Halpert G, Schimke LF, Ostrinski Y, Vojdani A, Baiocchi GC, et al. Autoantibodies targeting GPCRs and RAS-related molecules associate with COVID-19 severity. Nat Commun. 2022;13(1):1220. pmid:35264564
  21. 21. Skiba MA, Kruse AC. Autoantibodies as Endogenous Modulators of GPCR Signaling. Trends Pharmacol Sci. 2021;42(3):135–50. pmid:33358695
  22. 22. Dragun D, Philippe A, Catar R, Hegner B. Autoimmune mediated G-protein receptor activation in cardiovascular and renal pathologies. Thromb Haemost. 2009;101(4):643–8. pmid:19350106
  23. 23. Davenport AP, Hyndman KA, Dhaun N, Southan C, Kohan DE, Pollock JS, et al. Endothelin. Pharmacol Rev. 2016;68(2):357–418. pmid:26956245
  24. 24. Yanagisawa M, Kurihara H, Kimura S, Tomobe Y, Kobayashi M, Mitsui Y, et al. A novel potent vasoconstrictor peptide produced by vascular endothelial cells. Nature. 1988;332(6163):411–5. pmid:2451132
  25. 25. Kedzierski RM, Yanagisawa M. Endothelin system: the double-edged sword in health and disease. Annu Rev Pharmacol Toxicol. 2001;41:851–76. pmid:11264479
  26. 26. Kowalczyk A, Kleniewska P, Kolodziejczyk M, Skibska B, Goraca A. The role of endothelin-1 and endothelin receptor antagonists in inflammatory response and sepsis. Arch Immunol Ther Exp (Warsz). 2015;63(1):41–52. pmid:25288367
  27. 27. Hynynen MM, Khalil RA. The vascular endothelin system in hypertension--recent patents and discoveries. Recent Pat Cardiovasc Drug Discov. 2006;1(1):95–108. pmid:17200683
  28. 28. Park K-H, Park WJ, Han SJ, Kim H-S, Jo SH, Kim S-A, et al. Association Between Intra-arterial Invasive Central and Peripheral Blood Pressure and Endothelial Function (Assessed by Flow-Mediated Dilatation) in Stable Coronary Artery Disease. Am J Hypertens. 2019;32(10):953–9. pmid:31233098
  29. 29. Liu K, Cui R, Eshak ES, Cui M, Dong J-Y, Kiyama M, et al. Associations of central aortic pressure and brachial blood pressure with flow mediated dilatation in apparently healthy Japanese men: The Circulatory Risk in Communities Study (CIRCS). Atherosclerosis. 2017;259:46–50. pmid:28285093
  30. 30. Dimitropoulou C, White RE, Fuchs L, Zhang H, Catravas JD, Carrier GO. Angiotensin II relaxes microvessels via the AT(2) receptor and |Ca(2+)-activated K(+) (BK(Ca)) channels. Hypertension. 2001;37(2):301–7. pmid:11230289
  31. 31. Rosenbaum DM, Rasmussen SGF, Kobilka BK. The structure and function of G-protein-coupled receptors. Nature. 2009;459(7245):356–63. pmid:19458711
  32. 32. Yong SJ, Halim A, Halim M, Liu S, Aljeldah M, Al Shammari BR, et al. Inflammatory and vascular biomarkers in post-COVID-19 syndrome: A systematic review and meta-analysis of over 20 biomarkers. Rev Med Virol. 2023;33(2):e2424. pmid:36708022