Abstract
β-arrestins (βarrs), initially discovered as desensitizers of GPCR signaling, are now known to function as intracellular scaffolds and signaling transducers mediating a wide array of signaling cascades including immune responses to inflammatory stimuli. An important cause of immune cell infiltration and cardiac inflammation are viral pathogens such as enterovirus coxsackievirus B3 (CVB3) induced myocarditis. While viral myocarditis is a leading cause of dilated cardiomyopathy, the precise molecular mechanisms for the acute immune response to CVB3 infection are not well understood. Given the important role for βarrs in the acute immune response, we tested the hypothesis that βarrs are necessary for the activation of the acute immune response and mediate the progression and severity of cardiotropic CVB3-induced myocarditis in mice. Five to 7-week-old mice devoid of βarr1 (βarr1 KO) or βarr2 (βarr2 KO) were infected intraperitoneally with 1x103-1x104 plaque forming units (PFU) of CVB3 per animal. Wild type (WT) C57BL/6 mice infected with CVB3 were used as controls. The survival rate 7 days post infection (dpi) was significantly improved in male βarr1 KOs (80%) and βarr2 KOs (75%) compared to male WT control mice (35%, p=0.013). Female WT, βarr1 KO, and βarr2 KO mice showed similar survival rates 7 dpi., ranging from 70% to 80%. Early mortality among all groups before 5 dpi was associated with high viral titers (~6.0 ± 0.5 log10PFU/mg) in the liver compared to mortality after 5 dpi (~2.4 ± 1.7 log10PFU/mg) as determined by plaque assay. Viral titers in the heart (WT=3.7 ± 0.9 log10PFU/mg, βarr1KO=3.6 ± 1.3 log10PFU/mg, βarr2KO=3.5 ± 1.2log10PFU/mg) were similar among all groups suggesting that βarrs are not involved in viral replication. Morphometric analysis showed similar weight loss (~18%) across all groups at 7 dpi corroborated by viral cardiac PFU. Immunofluorescent staining of the heart with the pan-inflammatory marker, CD45, revealed high immune cell infiltration in infected WT mice (34.2% ± 4.5%), whereas immune cell infiltration was significantly blunted in infected βarr1 KO (6.0% ± 1.1%; p<0.0001) and βarr2 KO (8.5% ± 0.9%; p<0.0001) mice. The degree of immune cell infiltration in hearts of infected WT mice was directly correlated with an increase in heart viral titer, whereas immune cell infiltration remained blunted across a broad range of heart viral titers in both βarr1 and 2 KO mice. The blunted immune response in both βarr KOs compared to WT infected controls was consistent across multiple immune cell markers including CD4 for helper T cells and CD11b for innate immune cells. In conclusion, we demonstrate that βarrs are necessary for immune cell recruitment to the heart in CVB3 myocarditis and deletion of βarrs in male mice may be cardioprotective as indicated by an increase in survival rate. These data suggest that βarrs may serve as potential therapeutic targets in the treatment of acute viral myocarditis. This work was supported by the National Institutes of Health Grants HL056687 (to H.A.R.). This is the full abstract presented at the American Physiology Summit 2023 meeting and is only available in HTML format. There are no additional versions or additional content available for this abstract. Physiology was not involved in the peer review process.
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