Neuropsychiatric sequelae in an experimental model of post-COVID syndrome in mice

Jordane Clarisse Pimenta,Vinicius Amorim Beltrami,Bruna Da Silva Oliveira,Celso Martins Queiroz-Junior, Jessica Barsalini,Danielle Cunha Teixeira, Luiz Pedro Souza-Costa, Anna Luiza Diniz Lima,Caroline Amaral Machado, Barbara Zuccolotto Schneider Guimaraes Parreira,Felipe Rocha da Silva Santos, Pedro Augusto Carvalho Costa,Larisse De Souza Barbosa Lacerda, Mateus Rodrigues Goncalves,Ian de Meira Chaves, Manoela Gonzaga Gontijo Couto,Victor Rodrigues de Melo Costa, Natalia Ribeiro Cabacinha Nobrega, Barbara Luisa Silva, Talita Fonseca, Filipe Resende,Natalia Teixeira Wnuk, Hanna L Umezu,Gabriel Campolina-Silva,Ana Claudia Andrade,Renato Santana de Aguiar,Guilherme Mattos Jardim Costa,Pedro Pires Guimaraes, Glauber Santos Ferreira Silva,Luciene Bruno Vieira,Vanessa Pinho,Antonio Lucio Teixeira,Mauro Martins Teixeira, Aline Silva Miranda,Vivian Vasconcelos Costa

biorxiv(2024)

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摘要
The global impact of the COVID-19 pandemic has been unprecedented, and presently, the world is facing a new challenge known as Post-COVID syndrome (PCS). Current estimates suggest that more than 65 million people are grappling with PCS, encompassing several manifestations, including pulmonary, musculoskeletal, metabolic, and neuropsychiatric sequelae (cognitive and behavioral). The mechanisms underlying PCS remain unclear. The present study aimed to: (i) comprehensively characterize the acute effects of pulmonary inoculation of the betacoronavirus MHV-A59 in immunocompetent mice at clinical, cellular, and molecular levels; (ii) examine potential acute and long-term pulmonary, musculoskeletal, and neuropsychiatric sequelae induced by the betacoronavirus MHV-A59; and to (iii) assess sex-specific differences. Male and female C57Bl/6 mice were initially inoculated with varying viral titers (3x10^3 to 3x105 PFU/30 uL) of the betacoronavirus MHV-A59 via the intranasal route to define the highest inoculum capable of inducing disease without causing mortality. Further experiments were conducted with the 3x10^4 PFU inoculum. Mice exhibited an altered neutrophil/lymphocyte ratio in the blood in the 2nd and 5th day post-infection (dpi). Marked lung lesions were characterized by hyperplasia of the alveolar walls, infiltration of polymorphonuclear leukocytes (PMN) and mononuclear leukocytes, hemorrhage, increased concentrations of CCL2, CCL3, CCL5, and CXCL1 chemokines, as well as high viral titers until the 5th dpi. While these lung inflammatory signs resolved, other manifestations were observed up to the 60 dpi, including mild brain lesions with gliosis and hyperemic blood vessels, neuromuscular dysfunctions, anhedonic-like behavior, deficits in spatial working memory, and short-term aversive memory. These musculoskeletal and neuropsychiatric complications were exclusive to female mice and were prevented after ovariectomy. In summary, our study describes for the first time a novel sex-dependent model of PCS focused on neuropsychiatric and musculoskeletal disorders. This model provides a unique platform for future investigations regarding the effects of acute therapeutic interventions on the long-term sequelae unleashed by betacoronavirus infection. ### Competing Interest Statement The authors have declared no competing interest.
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