AI Article Synopsis
- The E6 protein from high-risk HPV (like HPV16) helps cancer cells grow by messing with a key protein called p53 that normally helps kill bad cells.
- Researchers found that E6 from HPV16 attaches to another protein called AIF, which helps cause cell death, and lowers its levels, making it harder for cells to die.
- Unlike E6 from HPV16, E6 from a non-cancer type (HPV6) doesn't lower the AIF levels, showing that the two types of E6 act differently in the body.
Article Abstract
Oncoprotein E6 of high-risk human papillomavirus (HPV) plays a critical role in inducing cell immortalization and malignancy. E6 downregulates caspase-dependent pathway through the degradation of p53. However, the effect of HPV E6 on other pathways is still under investigation. In the present study, we found that HPV E6 directly binds to all three forms (precursor, mature, and apoptotic) of apoptosis-inducing factor (AIF) and co-localizes with apoptotic AIF. This binding induced MG132-sensitive reduction of AIF expression in the presence of E6 derived from HPV16 (16E6), a cancer-causing type of HPV. Conversely, E6 derived from a non-cancer-causing type of HPV, HPV6 (6E6), did not reduce the levels of AIF despite its interaction with AIF. Flow cytometric analysis revealed that 16E6, but not 6E6, suppressed apoptotic AIF-induced chromatin degradation (an indicator of caspase-independent apoptosis) and staurosporine (STS, a protein kinase inhibitor)-induced apoptosis. AIF knockdown reduced STS-induced apoptosis in both of 16E6-expressing and 6E6-expressing cells; however, the reduction in 16E6-expressing cells was lower than that in 6E6-expressing cells. These findings indicate that 16E6, but not 6E6, blocks AIF-mediated apoptosis, and that AIF may represent a novel therapeutic target for HPV-induced cervical cancer.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7450093 | PMC |
| http://dx.doi.org/10.1038/s41598-020-71134-3 | DOI Listing |
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