Integrative Systems Immunology Analysis Reveals Elevated Anti-AGTR1 Levels with Accumulating COVID-19 Symptoms

  1. Dennyson Leandro M Fonseca
  2. Maj Jäpel
  3. Igor Salerno Filgueiras
  4. Gabriela Crispim Baiochi
  5. Yuri Ostrinski
  6. Gilad Halpert
  7. Yael Bublil Lavi
  8. Elroy Vojdani
  9. Juan Carlo Santos e Silva
  10. Júlia Nakanishi Usuda
  11. Paula P. Freire
  12. Adriel Leal Nóbile
  13. Anny Silva Adri
  14. Pedro Barcelos Marçal
  15. Yohan Lucas Gonçalves Corrêa
  16. Fernando Yuri Nery do Vale
  17. Letícia Oliveira Lopes
  18. Solveig Lea Schmidt
  19. Xiaoqing Wang
  20. Carl Vahldieck
  21. Benedikt Fels
  22. Lena F. Schimke
  23. Mario Hiroyuki Hirata
  24. Gustavo Cabral- Miranda
  25. Taj Ali AKhan
  26. Rusan Catar
  27. Guido Moll
  28. Thayna Silva-Sousa
  29. Yen-Rei A Yu
  30. Rodrigo JS Dalmolin
  31. Howard Amital
  32. Aristo Vojdani
  33. Helder Nakaya
  34. Hans D. Ochs
  35. Jonathan I. Silverberg
  36. Jason Zimmerman
  37. Israel Zyskind
  38. Avi Z Rosenberg
  39. Kai Schulze-Forster
  40. Harald Heidecke
  41. Alexander Hackel
  42. Kristina Kusche-Vihrog
  43. Yehuda Shoenfeld
  44. Gabriela Riemekasten
  45. Reza Akbarzadeh
  46. Alexandre H.C Marques
  47. Otavio Cabral-Marques
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Abstract

The coronavirus disease 2019 (COVID-19) displays a broad spectrum of symptoms, with the underlying reasons for this variability still not fully elucidated. Our study investigates the potential association between specific autoantibodies (AABs), notably those that targeting G protein-coupled receptors (GPCRs) and renin-angiotensin system (RAS) related molecules, and the diverse clinical manifestations of COVID-19, commonly observed in patients with autoimmune conditions, including rheumatic diseases, such as systemic sclerosis. In a cross-sectional analysis, we explored the relationship between AAB levels and the presence of key COVID-19 symptoms. Hierarchical clustering analysis revealed a robust correlation between certain AABs and symptoms such as fever, muscle ache, anosmia, and dysgeusia, which emerged as significant predictors of disease severity. Specifically, AABs against CHRM5 and CXCR3 were strongly linked to fever, while AABs against CHRM5 and BDKRB1 correlated with muscle ache. Anosmia was predominantly associated with AABs against F2R and AGTR1, while dysgeusia was linked to AABs against BDKRB1 and AGTR1. Furthermore, we observed a rise in AAB levels with the accumulation of these symptoms, with the highest levels detected in patients presenting all four predictors. Multinomial regression analysis identified AABs targeting AGTR1 as a key predictor for one or more of these core symptoms. Additionally, our study indicated that anti-AGTR1 antibodies triggered a concentration-dependent degradation of eGC, which could be mitigated by the AGTR1 antagonist Losartan. This suggests a potential mechanistic connection between eGC degradation, the observed COVID-19 symptoms, and rheumatic diseases. In conclusion, our research underscores a substantial correlation between AABs, particularly those against GPCRs and RAS-related molecules, and the severity of COVID-19 symptoms. These findings open avenues for potential therapeutic interventions in the management of COVID-19.

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  1. Version published to 10.1101/2024.04.05.24305287v1 on medRxiv