HIV-1 exploits Hes-1 expression during pre-existing HPV-16 infection for cancer progression.

Q2 Medicine VirusDisease Pub Date : 2023-03-01 Epub Date: 2023-02-08 DOI:10.1007/s13337-023-00809-y

Serena D'Souza, Arati Mane, Linata Patil, Aazam Shaikh, Madhuri Thakar, Vandana Saxena, Leila Fotooh Abadi, Sheela Godbole, Smita Kulkarni, Raman Gangakhedkar, Padma Shastry, Samiran Panda

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Abstract

High Risk Human Papilloma Viruses (HR-HPV) persistently infect women with Human Immunodeficiency Virus-1 (HIV-1). HPV-16 escapes immune surveillance in HIV-1 positive women receiving combined antiretroviral therapy (cART). HIV-1 Tat and HPV E6/E7 proteins exploit Notch signaling. Notch-1, a developmentally conserved protein, influences cell fate from birth to death. Notch-1 and its downstream targets, Hes-1 and Hey-1 contribute to invasive and aggressive cancers. Cervical cancer cells utilize Notch-1 and hyper-express CXCR4, a co-receptor of HIV-1. Accumulating evidence shows that HIV-1 affects cell cycle progression in pre-existing HPV infection. Additionally, Tat binds Notch-1 receptor for activation and influences cell proliferation. Oncogenic viruses may interfere or converge together to favor tumor growth. The molecular dialogue during HIV-1/HPV-16⁺ co-infections in the context of Notch-1 signaling has not been explored thus far. This in vitro study was designed with cell lines (HPV-ve C33A and HPV-16⁺ CaSki) which were transfected with plasmids (pLEGFPN1 encoding HIV-1 Tat and pNL4-3 encoding HIV-1 [full HIV-1 genome]). HIV-1 Tat and HIV-1 inhibited Notch-1expression, with differential effects on EGFR. Notch-1 inhibition nullified Cyclin D expression with p21 induction and increased G₂-M cell population in CaSki cells. On the contrary, HIV-1 infection shuts down p21 expression through interaction of Notch-1 downstream genes Hes-1-EGFR and Cyclin D for G₂-M arrest, DDR response and cancer progression. This work lays foundations for future research and interventions, and therefore is necessary. Our results describe for the first time how HIV-1 Tat cancers have an aggressive nature due to the interplay between Notch-1 and EGFR signaling. Notch-1 inhibitor, DAPT used in organ cancer treatment may help rescue HIV-1 induced cancers.

Graphical abstract: The illustration shows how HIV interacts with HPV-16 to induce Notch 1 suppression for cancer progression (Created with BioRender.com).

Supplementary information: The online version contains supplementary material available at 10.1007/s13337-023-00809-y.

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艾滋病毒-1利用HPV-16感染前的Hes-1表达促进癌症进展。

高危人乳头瘤病毒（HR-HPV）会持续感染感染人类免疫缺陷病毒-1（HIV-1）的妇女。在接受联合抗逆转录病毒疗法（cART）的 HIV-1 阳性妇女中，HPV-16 可逃避免疫监视。HIV-1 Tat 和 HPV E6/E7 蛋白利用了 Notch 信号转导。Notch-1是一种发育保守的蛋白质，影响着细胞从出生到死亡的命运。Notch-1及其下游靶标Hes-1和Hey-1会导致侵袭性和侵袭性癌症。宫颈癌细胞利用 Notch-1 并过度表达 HIV-1 的共受体 CXCR4。越来越多的证据表明，HPV 感染前，HIV-1 会影响细胞周期的进展。此外，Tat 与 Notch-1 受体结合激活并影响细胞增殖。致癌病毒可能会相互干扰或共同作用，以促进肿瘤生长。迄今为止，还没有人探讨过 HIV-1/HPV-16+ 共同感染时，在 Notch-1 信号传导背景下的分子对话。这项体外研究设计的细胞系（HPV-ve C33A 和 HPV-16+ CaSki）转染了质粒（编码 HIV-1 Tat 的 pLEGFPN1 和编码 HIV-1 [HIV-1 全基因组] 的 pNL4-3）。HIV-1 Tat和HIV-1抑制了Notch-1的表达，并对表皮生长因子受体产生了不同的影响。在 CaSki 细胞中，Notch-1 的抑制使 Cyclin D 的表达无效，并诱导 p21 和增加 G2-M 细胞数量。相反，HIV-1感染会通过Notch-1下游基因Hes-1-EGFR和Cyclin D的相互作用抑制p21的表达，从而导致G2-M停滞、DDR反应和癌症进展。这项工作为未来的研究和干预奠定了基础，因此非常必要。我们的研究结果首次描述了 HIV-1 Tat 癌症如何因 Notch-1 和表皮生长因子受体信号的相互作用而具有侵袭性。用于器官癌症治疗的Notch-1抑制剂DAPT可能有助于挽救HIV-1诱导的癌症。图解摘要：图解显示了HIV如何与HPV-16相互作用，诱导Notch 1抑制癌症进展（使用BioRender.com创建）：在线版本包含补充材料，可查阅 10.1007/s13337-023-00809-y。

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来源期刊

VirusDisease Medicine-Infectious Diseases

CiteScore

7.00

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0.00%

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期刊介绍： VirusDisease, formerly known as ''Indian Journal of Virology'', publishes original research on all aspects of viruses infecting animal, human, plant, fish and other living organisms.