Anticipating the Next Chess Move: Blocking SARS-CoV-2 Replication and Simultaneously Disarming Viral Escape Mechanisms

Samir Mansour Moraes Casseb; André Salim Khayat; Jorge Estefano Santana de Souza; Edivaldo Herculano Correa de Oliveira; Sidney Emanuel Batista Dos Santos; Pedro Fernando da Costa Vasconcelos; Paulo Pimentel de Assumpção

doi:10.3390/genes13112147

Anticipating the Next Chess Move: Blocking SARS-CoV-2 Replication and Simultaneously Disarming Viral Escape Mechanisms

Genes (Basel). 2022 Nov 18;13(11):2147. doi: 10.3390/genes13112147.

Authors

Samir Mansour Moraes Casseb¹, André Salim Khayat¹, Jorge Estefano Santana de Souza², Edivaldo Herculano Correa de Oliveira¹, Sidney Emanuel Batista Dos Santos¹, Pedro Fernando da Costa Vasconcelos³, Paulo Pimentel de Assumpção¹

Affiliations

¹ Oncology Research Center, Federal University of Pará, Belém 66073-000, Brazil.
² Bioinformatics Graduate Program, Metrópole Digital Institute, Federal University of Rio Grande do Norte Natal, Natal 59078-400, Brazil.
³ Department of Pathology, Pará State University, Belém 66087-670, Brazil.

Abstract

The COVID-19 pandemic initiated a race to determine the best measures to control the disease and to save as many people as possible. Efforts to implement social distancing, the use of masks, and massive vaccination programs turned out to be essential in reducing the devastating effects of the pandemic. Nevertheless, the high mutation rates of SARS-CoV-2 challenge the vaccination strategy and maintain the threat of new outbreaks due to the risk of infection surges and even lethal variations able to resist the effects of vaccines and upset the balance. Most of the new therapies tested against SARS-CoV-2 came from already available formulations developed to treat other diseases, so they were not specifically developed for SARS-CoV-2. In parallel, the knowledge produced regarding the molecular mechanisms involved in this disease was vast due to massive efforts worldwide. Taking advantage of such a vast molecular understanding of virus genomes and disease mechanisms, a targeted molecular therapy based on siRNA specifically developed to reach exclusive SARS-CoV-2 genomic sequences was tested in a non-transformed human cell model. Since coronavirus can escape from siRNA by producing siRNA inhibitors, a complex strategy to simultaneously strike both the viral infectious mechanism and the capability of evading siRNA therapy was developed. The combined administration of the chosen produced siRNA proved to be highly effective in successfully reducing viral load and keeping virus replication under control, even after many days of treatment, unlike the combinations of siRNAs lacking this anti-anti-siRNA capability. Additionally, the developed therapy did not harm the normal cells, which was demonstrated because, instead of testing the siRNA in nonhuman cells or in transformed human cells, a non-transformed human thyroid cell was specifically chosen for the experiment. The proposed siRNA combination could reduce the viral load and allow the cellular recovery, presenting a potential innovation for consideration as an additional strategy to counter or cope COVID-19.

Keywords: COVID-19; SARS-CoV-2; siRNA; treatment.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

COVID-19*
Genome, Viral
Humans
Pandemics
RNA, Small Interfering / genetics
SARS-CoV-2* / genetics
Virus Replication / genetics

Substances

RNA, Small Interfering

Grants and funding

This research was funded by the Federal University of Pará (UFPA).