The ATG5 interactome links clathrin-mediated vesicular trafficking with the autophagosome assembly machinery

Baines, Kiren; Yoshioka, Kazuaki; Takuwa, Yoh; Lane, Jon D.

doi:10.1080/27694127.2022.2042054

Cited by 13 publications

(11 citation statements)

References 77 publications

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“…Our model hypothesizes that ATG5 engages specific forms of BST2 tethered to virions to an LC3C-associated pathway, in which endosomal structures are customized by some ATG proteins. Interestingly, recent proteomic approaches described a strong link between ATG5 and clathrin adaptor protein complexes (AP)-dependent endocytic pathway ( 41 ). Moreover, several studies reported that Vpu/BST2 complex can interact with the AP complexes and that these interactions are important for BST2 antagonism by Vpu ( 11 ).…”

Section: Discussionmentioning

confidence: 99%

ATG5 selectively engages virus-tethered BST2/tetherin in an LC3C-associated pathway

Judith

Versapuech

Bejjani

et al. 2023

Proc. Natl. Acad. Sci. U.S.A.

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Bone marrow stromal antigen 2 (BST2)/tetherin is a restriction factor that reduces HIV-1 dissemination by tethering virus at the cell surface. BST2 also acts as a sensor of HIV-1 budding, establishing a cellular antiviral state. The HIV-1 Vpu protein antagonizes BST2 antiviral functions via multiple mechanisms, including the subversion of an LC3C-associated pathway, a key cell intrinsic antimicrobial mechanism. Here, we describe the first step of this viral-induced LC3C-associated process. This process is initiated at the plasma membrane through the recognition and internalization of virus-tethered BST2 by ATG5, an autophagy protein. ATG5 and BST2 assemble as a complex, independently of the viral protein Vpu and ahead of the recruitment of the ATG protein LC3C. The conjugation of ATG5 with ATG12 is dispensable for this interaction. ATG5 recognizes cysteine-linked homodimerized BST2 and specifically engages phosphorylated BST2 tethering viruses at the plasma membrane, in an LC3C-associated pathway. We also found that this LC3C-associated pathway is used by Vpu to attenuate the inflammatory responses mediated by virion retention. Overall, we highlight that by targeting BST2 tethering viruses, ATG5 acts as a signaling scaffold to trigger an LC3C-associated pathway induced by HIV-1 infection.

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Section: Discussionmentioning

confidence: 99%

ATG5 selectively engages virus-tethered BST2/tetherin in an LC3C-associated pathway

Judith

Versapuech

Bejjani

et al. 2023

Proc. Natl. Acad. Sci. U.S.A.

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“…Interestingly, recent proteomic approaches described strong link between ATG5 and clathrin adaptor protein complexes (AP)-dependent endocytic pathway (41). Moreover, several studies reported that Vpu/BST2 complex can interact with the AP complexes and that these interactions are important for BST2 antagonism by Vpu (11).…”

Section: Discussionmentioning

confidence: 99%

“…Our model hypothesizes that ATG5 engages specific forms of BST2 tethered to virions to an LC3C-associated pathway, in which endosomal structures are customized by some ATG proteins. Interestingly, recent proteomic approaches described strong link between ATG5 and clathrin adaptor protein complexes (AP)-dependent endocytic pathway (41). Moreover, several studies reported that Vpu/BST2 complex can interact with the AP complexes and that these interactions are important for BST2 antagonism by Vpu (11).…”

Section: Discussionmentioning

confidence: 99%

ATG5 selectively engages virus-tethered BST2/Tetherin in an LC3C-associated pathway

Judith

Versapuech

Bejjani

et al. 2023

Preprint

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BST2/Tetherin is a restriction factor that reduces HIV-1 dissemination by tethering virus at the cell surface. BST2 also acts as a sensor of HIV-1 budding, establishing a cellular anti-viral state. The HIV-1 Vpu protein antagonizes BST2 antiviral functions, notably by subverting an LC3C-associated pathway, a key cell intrinsic anti-microbial mechanism. Here, we show that ATG5 associates with BST2 and acts as a signaling scaffold to trigger an LC3C-associated pathway induced by HIV-1 infection. This process is initiated at the plasma membrane through the recognition of virus-tethered BST2 by ATG5. ATG5 and BST2 assemble as a complex, independently of the viral protein Vpu and ahead of the recruitment of the ATG protein LC3C. The conjugation of ATG5 with ATG12 is dispensable for this interaction. ATG5 recognizes cysteine-linked homodimerized BST2 and specifically engages phosphorylated BST2 tethering viruses at the plasma membrane, in an LC3C-associated pathway. We also found that this LC3C-associated pathway is used by Vpu to attenuate the inflammatory responses mediated by virion retention. Overall, we highlight that by targeting BST2 tethering viruses, ATG5 acts as a transducer of the LC3C-associated pathway induced by HIV-1 infection.

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“…This complex is localized on the outer membrane surface of the preautophagosomal structure and is involved in the expansion of the preautophagosomal outer membrane. Impaired activation of ATG5 and ATG12 often leads to impaired cellular autophagy [33][34][35] . BCL2L1 is a well-known anti-apoptotic protein, and it has been shown that BCL2L1 can inhibit autophagy by binding to beclin1 protein, which regulates the assembly of phagosomal membranes during autophagy 36,37 .…”

Section: Discussionmentioning

confidence: 99%

Dysregulated autophagy-related genes in abdominal aortic aneurysm: Comprehensive bioinformatics analysis and experimental validation

Xie

Shen

Wang

et al. 2022

Preprint

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Background Abdominal aortic aneurysm (AAA) is a serious life-threatening cardiovascular disease that occurs in middle-aged and elderly people. Previous experimental studies have suggested that autophagy may be involved in the pathological process of AAA, but the pathogenesis of autophagy in AAA is unclear. We aim to identify and validate key potential autophagy-related genes involved in AAA through bioinformatics analysis to further elucidate the mechanisms of autophagy dysregulation in AAA. Methods The GSE57691 microarray dataset was downloaded from the Gene Expression Omnibus database (GEO), including 49 AAA samples and 10 normal aortic samples. 232 autophagy-related genes were obtained from the Human Autophagy Database (HADb). The GSE57691 dataset was crossed with the autophagy gene set to screen for differentially expressed autophagy-related genes (DE-ARGs) involved in AAA. In addition, gene ontology (GO) and Kyoto Encyclopedia of Genes and Genomes (KEGG) pathway enrichment analyses were performed on the DE-ARGs in AAA using R software. Protein-protein interaction (PPI) networks were constructed using the STRING database, significant gene cluster modules were identified using the MCODE Cytoscape plugin, and hub genes in AAA associated DE-ARGs were screened using the CytoHubba Cytospace plugin. Meanwhile, DE-ARGs were calculated using the least absolute shrinkage selection algorithm (LASSO) algorithm. By crossing the LASSO calculation results and hub genes, the final key genes were identified, whose expression levels were further validated in AAA aortic samples by qRT-PCR. Finally, the transcription factor regulatory networks and target drugs of these key genes were predicted by the JASPAR database and DsigDB database, respectively. Results A total of 57 DE-ARGs were identified in aortic samples from normal controls and AAA. GO and KEGG analysis showed that these 57 DE-ARGs involved in AAA were particularly enriched in macroautophagy, PI3K-Akt signaling pathway, AMPK signaling pathway, and apoptosis. PPI results indicated that the 57 DE-ARGs interacted with each other. A total of 6 key genes (ATG5, ATG12, MTOR, BCL2L1, EIF4EBP1, and RPTOR) were identified using CytoHubba and LASSO algorithms. Detection of clinical samples by qRT-PCR indicated that ATG5, ATG12, BCL2L1, EIF4EBP1, and RPTOR expression was consistent with bioinformatic analysis. A regulatory network containing 6 key genes and 30 transcription factors was constructed through the JASPAR database. Finally, four targeted autophagy regulatory drugs, rapamycin, Temsirolimus, Sorafenib, and NVP-BEZ235, were screened by the DsigDB database. Conclusions Bioinformatics analysis identified 57 autophagy-related genes that may be involved in AAA. ATG5, ATG12, BCL2L1, EIF4EBP1and RPTOR may serve as potential drug targets and biomarkers as they regulate autophagy. These results expand the understanding of autophagy dysfunction in AAA and may contribute to the diagnosis and prognosis of AAA.

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The ATG5 interactome links clathrin-mediated vesicular trafficking with the autophagosome assembly machinery

Cited by 13 publications

References 77 publications

ATG5 selectively engages virus-tethered BST2/tetherin in an LC3C-associated pathway

ATG5 selectively engages virus-tethered BST2/tetherin in an LC3C-associated pathway

ATG5 selectively engages virus-tethered BST2/Tetherin in an LC3C-associated pathway

Dysregulated autophagy-related genes in abdominal aortic aneurysm: Comprehensive bioinformatics analysis and experimental validation

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