Institut National de la Recherche Scientifique (INRS)-Centre Armand-Frappier Santé Biotechnologie.
The Sprott Center for Stem Cell Research, Regenerative Medicine Program, Ottawa Hospital Research Institute, Ottawa, ON, Canada.
Autophagy. 2021 Nov;17(11):3408-3423. doi: 10.1080/15548627.2021.1874134. Epub 2021 Jan 18.
Although macroautophagy/autophagy has been proposed as a critical defense mechanism against HIV-1 by targeting viral components for degradation, its contribution as a catabolic process in providing optimal anti-HIV-1 immunity has never been addressed. The failure to restore proper antiviral CD8A/CD8 T-cell immunity, especially against HIV-1, is still the major limitation of current antiretroviral therapies. Consequently, it is of clinical imperative to provide new strategies to enhance the function of HIV-1-specific CD8A T-cells in patients under antiretroviral treatments (ART). Here, we investigated whether targeting autophagy activity could be an optional solution to make this possible. Our data show that, after both polyclonal and HIV-1-specific activation, CD8A T-cells from ART displayed reduced autophagy-dependent degradation of lysosomal contents when compared to naturally HIV-1 protected elite controllers (EC). We further confirmed in EC, by using specific gene silencing and lysosomal inhibitors, the critical role of active autophagy in superior CD8A T-cell protection against HIV-1. More importantly, we found that an IL21 treatment was effective in rescuing the antiviral CD8A T-cell immunity from ART in an autophagy-dependent manner. Finally, we established that IL21-dependent rescue occurred due to the enhanced degradation of endogenous lipids via autophagy, referred to as lipophagy, which fueled the cellular rates of mitochondrial beta-oxidation. In summary, our data show that autophagy/lipophagy can be considered as a therapeutic tool to elicit functional antiviral CD8 T-cell responses. Our results also provide additional insights toward the development of improved T-cell-based prevention and cure strategies against HIV-1. ART: patients under antiretroviral therapy; BaF: bafilomycin A; BECN1: beclin 1; CEF: cytomegalo-, Epstein-Barr- and flu-virus peptide pool; Chloro.: chloroquine; EC: elite controllers; FAO: fatty acid beta-oxidation; HIV: HIV-1-uninfected control donors; IFNG/IFN-γ: interferon gamma; IL21: interleukin 21; MAP1LC3/LC3: microtubule associated protein 1 light chain 3; PBMC: peripheral blood mononuclear cells; SQSTM1: sequestosome 1; ULK1: unc-51 like autophagy activating kinase 1.
虽然自噬/自噬已被提议作为一种关键的防御机制,通过靶向病毒成分进行降解来抵抗 HIV-1,但它作为一种分解代谢过程,为提供最佳的抗 HIV-1 免疫贡献尚未得到解决。未能恢复适当的抗病毒 CD8A/CD8 T 细胞免疫,特别是针对 HIV-1,仍然是当前抗逆转录病毒疗法的主要限制。因此,提供新的策略来增强接受抗逆转录病毒治疗(ART)的患者中 HIV-1 特异性 CD8A T 细胞的功能具有临床必要性。在这里,我们研究了靶向自噬活性是否可以作为一种可行的解决方案。我们的数据表明,与自然感染 HIV-1 的精英控制者(EC)相比,ART 后的多克隆和 HIV-1 特异性激活后,CD8A T 细胞的溶酶体内容物的自噬依赖性降解减少。我们通过使用特定的基因沉默和溶酶体抑制剂进一步证实,在 EC 中,活跃的自噬在保护 HIV-1 特异性 CD8A T 细胞方面起着至关重要的作用。更重要的是,我们发现 IL21 治疗能够以自噬依赖的方式有效恢复来自 ART 的抗病毒 CD8A T 细胞免疫。最后,我们确定 IL21 依赖性恢复是由于自噬介导的内源性脂质的降解,称为脂自噬,这为线粒体β-氧化提供了细胞速率。总之,我们的数据表明,自噬/脂自噬可以被认为是一种治疗工具,以引发功能性抗病毒 CD8 T 细胞反应。我们的结果还为开发针对 HIV-1 的改进的基于 T 细胞的预防和治疗策略提供了额外的见解。ART:接受抗逆转录病毒治疗的患者;BaF:巴佛洛霉素 A;BECN1:beclin 1;CEF:巨细胞病毒、EBV 和流感病毒肽库;Chloro.:氯喹;EC:精英控制者;FAO:脂肪酸β-氧化;HIV:未感染 HIV-1 的对照供体;IFNG/IFN-γ:干扰素γ;IL21:白细胞介素 21;MAP1LC3/LC3:微管相关蛋白 1 轻链 3;PBMC:外周血单核细胞;SQSTM1:自噬相关蛋白 1 轻链 3;ULK1:UNC-51 样自噬激活激酶 1。
