Antiandrogens pose a protective effect against COVID-19 by boosting the human myxovirus resistance gene 1 (mx1)

Bizzotto, Juan Antonio; Sanchis, Pablo Antonio; Lavignolle, Rosario; Lage Vickers, Sofia; Sabater, Agustina Ayelen; Abbate, Mercedes; Toro, Ayelen Rayen; Anselmino, Nicolás; Labanca, Estefania; Navone, Nora; Vazquez, Elba Susana; Cotignola, Javier Hernan; Gueron, Geraldine

info:eu-repo/semantics/publishedVersion

Fecha

2021

Registro en:

Antiandrogens pose a protective effect against COVID-19 by boosting the human myxovirus resistance gene 1 (mx1); LXVI Reunión anual de la Sociedad Argentina de Investigación Clínica (SAIC); LXIX Reunión Anual de la Sociedad Argentina de Inmunología (SAI); LIII Reunión Anual de la Asociación Argentina de Farmacología Experimental (AAFE) y XI Reunión Anual de la Asociación Argentina de Nanomedicinas (NANOMED-AR); Argentina; 2021; 76-77

1669-9106

http://hdl.handle.net/11336/161434

CONICET Digital

CONICET

https://repositorioslatinoamericanos.uchile.cl/handle/2250/4410313

Autor

Bizzotto, Juan Antonio

Sanchis, Pablo Antonio

Lavignolle, Rosario

Lage Vickers, Sofia

Sabater, Agustina Ayelen

Abbate, Mercedes

Toro, Ayelen Rayen

Anselmino, Nicolás

Labanca, Estefania

Navone, Nora

Vazquez, Elba Susana

Cotignola, Javier Hernan

Gueron, Geraldine

Institución

Consejo Nacional de Investigaciones Científicas y Tecnológicas (Argentina)

Resumen

Population-based studies have shown that prostate cancer (PCa) patients undergoing androgen-deprivation therapies (ADT) were partially protected from COVID-19. Men treated with proxalutamide in a recent clinical trial showed reduced COVID-19 hospitalization rate. In this work we assessed gene expression profiles and androgen regulation of the main host cell receptors described for SARS-CoV-2 and potential antiviral genes involved in response to coronavirus infection.Multiple bioinformatics analyses were performed to study host cell receptors and antiviral proteins in SARS-CoV-2 infection and the gene expression changes upon ADT was assessed. We used publicly available datasets from: a) SARS-CoV-2 positive and negative patients? nasopharyngeal swabs at time of diagnosis (GSE152075, n=453), b) SARS-CoV-2 infected human cell lines and ferrets (GSE1407507), c) ChIP-seq experiments evaluating androgen receptor binding (GSE66037, GSE28950, GSE108704).Results showed that SARS-CoV-2 positive cases had higher MX1 expression, and multivariable regression showed that MX1 expression significantly increased with viral load. Also, MX1 was significantly up-regulated in tracheal samples from ferrets intranasally infected with SARS-CoV-2. Similar results were found in A549 and Calu3 lung cell lines. Since ADT might result in a therapeutic advantage against COVID-19, we next evaluated MX1 regulation by dihydrotestosterone (DHT). First, comparable MX1 levels in lung, prostate and salivary gland of healthy humans were observed (GTEx). LNCaP cells treated with DHT showed a decrease (p<0.05) in MX1 mRNA levels. ChIP-seq experiments showcased AR binding sites on the MX1 sequence upon DHT. Further, comparison of paired PCa patient?s samples before and after ADT showed MX1 upregulation (p<0.05) after ADT.In summary, MX1 raises as a critical responder in SARS-CoV-2 infection and we demonstrate MX1 modulation by DHT. We propose MX1 as a key player in the therapeutic advantage posed by ADT.

Materias

antiandrogens

COVID-19

mx1

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