<p>The SARS-CoV-2 virus, which causes Covid-19, may hijack our cells' internal cholesterol processing system to help it spread through the body, according to a study which hints at new targets for a potential therapy against the disease.</p>.<p>The cell culture study, published in the journal <em>Nature Metabolism</em>, identifies a potential molecular connection between cholesterol metabolism and Covid-19.</p>.<p>The researchers from the Academy of Military Medical Sciences (AMMS) in China found that the SARS-CoV-2 virus sticks to a receptor on the human cells that usually binds to HDL cholesterol, also known as 'good' cholesterol.</p>.<p>When the scientists blocked the cholesterol receptor in the cells, the virus was no longer able to stick to them.</p>.<p><strong><a href="www.deccanherald.com/national/coronavirus-news-live-updates-india-world-coronavirus-vaccine-karnataka-maharashtra-tamil-nadu-delhi-kerala-gujarat-bengal-bengaluru-mumbai-new-delhi-chennai-kolkata-cases-deaths-recoveries-Covid-19-vaccine-920349.html#1">For latest updates on Coronavirus outbreak, click here</a></strong></p>.<p>They say this hints at new targets for treatment, although this is very early-stage research.</p>.<p>The study suggests that SARS-CoV-2 may use the cell's internal cholesterol mechanisms to enhance infection.</p>.<p>During SARS-CoV-2 infection, the spike protein on the virus binds a host-cell receptor called angiotensin-converting enzyme 2 (ACE2).</p>.<p>The researchers highlight the role of another receptor, called HDL scavenger receptor B type 1 (SR-B1), which is expressed in several tissues, including human lung cells.</p>.<p>This receptor usually binds high-density lipoprotein (HDL).</p>.<p>However, in this study, the viral spike protein-bound cholesterol, and expression of SR-B1 and the presence of HDL together helped the virus bind and enter ACE2-expressing cells.</p>.<p>The virus seems to hijack the cell's cholesterol-uptake machinery to facilitate entry into host cells, but when the researchers blocked this pathway with a monoclonal antibody or a specific pharmacological antagonist of SR-B1, the HDL-mediated enhancement of viral infection was absent.</p>.<p>They conclude that the study highlights a potential molecular connection between Covid-19 and cholesterol, and they suggest that drugs targeting SR-B1 may help limit SARS-CoV-2 infection.</p>
<p>The SARS-CoV-2 virus, which causes Covid-19, may hijack our cells' internal cholesterol processing system to help it spread through the body, according to a study which hints at new targets for a potential therapy against the disease.</p>.<p>The cell culture study, published in the journal <em>Nature Metabolism</em>, identifies a potential molecular connection between cholesterol metabolism and Covid-19.</p>.<p>The researchers from the Academy of Military Medical Sciences (AMMS) in China found that the SARS-CoV-2 virus sticks to a receptor on the human cells that usually binds to HDL cholesterol, also known as 'good' cholesterol.</p>.<p>When the scientists blocked the cholesterol receptor in the cells, the virus was no longer able to stick to them.</p>.<p><strong><a href="www.deccanherald.com/national/coronavirus-news-live-updates-india-world-coronavirus-vaccine-karnataka-maharashtra-tamil-nadu-delhi-kerala-gujarat-bengal-bengaluru-mumbai-new-delhi-chennai-kolkata-cases-deaths-recoveries-Covid-19-vaccine-920349.html#1">For latest updates on Coronavirus outbreak, click here</a></strong></p>.<p>They say this hints at new targets for treatment, although this is very early-stage research.</p>.<p>The study suggests that SARS-CoV-2 may use the cell's internal cholesterol mechanisms to enhance infection.</p>.<p>During SARS-CoV-2 infection, the spike protein on the virus binds a host-cell receptor called angiotensin-converting enzyme 2 (ACE2).</p>.<p>The researchers highlight the role of another receptor, called HDL scavenger receptor B type 1 (SR-B1), which is expressed in several tissues, including human lung cells.</p>.<p>This receptor usually binds high-density lipoprotein (HDL).</p>.<p>However, in this study, the viral spike protein-bound cholesterol, and expression of SR-B1 and the presence of HDL together helped the virus bind and enter ACE2-expressing cells.</p>.<p>The virus seems to hijack the cell's cholesterol-uptake machinery to facilitate entry into host cells, but when the researchers blocked this pathway with a monoclonal antibody or a specific pharmacological antagonist of SR-B1, the HDL-mediated enhancement of viral infection was absent.</p>.<p>They conclude that the study highlights a potential molecular connection between Covid-19 and cholesterol, and they suggest that drugs targeting SR-B1 may help limit SARS-CoV-2 infection.</p>