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Részletek

A cikk állandó MOB linkje:
http://mob.gyemszi.hu/detailsperm.jsp?PERMID=148821
MOB:2021/1
Szerzők:Székács B.; Várbíró Sz.; Debreczeni L.
Tárgyszavak:KORONAVÍRUS; SARS-COV-2; PANDEMIA; ACE - GÁTLÓK (ANGIOTENZIN-KONVERTÁLÓ ENZIM INHIBITOROK); BRADYKININ; RECEPTOROK; LÉGZÉSI DISTRESSZ SZINDRÓMA, FELNŐTTNÉL
Folyóirat:Physiology International - 2021. 108. évf. 1. sz.
[https://akjournals.com/view/journals/2060/2060-overview.xml]


  High-dose ACEi might be harmful in COVID-19 patients with serious respiratory distress syndrome by leading to excessive bradykinin receptor activation / B. Székács, Sz. Várbíró, L. Debreczeni
  Bibliogr.: p. 7-9. - Abstr. eng. - DOI: https://doi.org/10.1556/2060.2021.00007
  In: Physiology International. - ISSN 2498-602X, eISSN 2677-0164. - 2021. 108. évf. 1. sz., p. 1-9. : ill.


Purpose: We aimed to critically review the available information on the potential contribution of excessive kallikrein-kinin systems (KKSs) activation to severe respiratory inflammation in SARS-CoV-2 infection, and the likely consequence of ACE inhibition in seriously affected patients. Methods: The literature related to the above topic was reviewed including papers that analysed the connections, actions, interactions, consequences and occasionally suggestions for rational interventions. Results/Conclusion: Severe bronchoalveolar inflammation seems to be caused, at least in part, by upregulation of the KKS that increases plasma and/or local tissue concentrations of bradykinin (BK) in patients with COVID-19 infection. Besides KKS activation, suppression of ACE activity results in decreased bradykinin degradation, and these changes in concert can lead to excessive BK B1 and B2 receptor (BKB1R/BKB2R) activation. Aminopeptidase P (APP), and carboxypeptidase N also degrade bradykinin, but their protein expression and activity are unclear in COVID-19 infection. On the other hand, ACE2 expression is upregulated in patients with COVID-19 infection, so ACE2 activity is unlikely to be decreased despite blockade of part of ACE2 by the virus for entry into the cells. ACE2 cleaves lys-des-arginine9BK and arg-des-arginine9BK, the active metabolites of bradykinin, which stimulate the BKB1R receptor. Stimulation of BKB1R/BKB2R can exacerbate the pulmonary inflammatory response by causing vascular leakage and edema, vasodilation, smooth muscle spasm and stimulation of pain afferent nerves. Despite all uncertainties, it seems rational to treat comorbid COVID patients with serious respiratory distress syndrome with ARBs instead of high-dose ACE inhibitor (ACEi) that will further decrease bradykinin degradation and enhance BKB1R/BKB2R activation, but ACEi may not be contraindicated in patients with mild pulmonary symptoms.  Kulcsszavak: COVID-19, cardiovascular, respiratory inflammation, RAS, ACE2, kallikrein-kinin system, bradykinin, ACE-inhibitor, angiotensin receptor blocker, old patient, hypertension

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