The Role of Autophagy and Autophagy Receptor NDP52 in Microbial Infections

Fan, Songqing; Wu, Keke; Zhu, Erpeng; Ma, Shuaipeng; Chen, Yuming; Ding, Hongxing; Yi, Lin; Zhao, Mingqiu; Chen, Jinding

doi:10.3390/ijms21062008

Cited by 15 publications

(15 citation statements)

References 99 publications

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“…Human NDP52 consists of the SKIP carboxyl homology (SKICH), LC3-interacting region (LIR), coiled-coil, galectin-8 binding (GALBI), and C-terminal ubiquitin-binding zinc finger (UBZ) domains ( 17 , 19 ) ( Figure 1A ). The substitution of Asp439 by Arg (D439R) in the UBZ domain reportedly abolishes the ubiquitin-binding ( 31 ).…”

Section: Resultsmentioning

confidence: 99%

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Crosstalk Between NDP52 and LUBAC in Innate Immune Responses, Cell Death, and Xenophagy

et al. 2021

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Nuclear dot protein 52 kDa (NDP52, also known as CALCOCO2) functions as a selective autophagy receptor. The linear ubiquitin chain assembly complex (LUBAC) specifically generates the N-terminal Met1-linked linear ubiquitin chain, and regulates innate immune responses, such as nuclear factor-κB (NF-κB), interferon (IFN) antiviral, and apoptotic pathways. Although NDP52 and LUBAC cooperatively regulate bacterial invasion-induced xenophagy, their functional crosstalk remains enigmatic. Here we show that NDP52 suppresses canonical NF-κB signaling through the broad specificity of ubiquitin-binding at the C-terminal UBZ domain. Upon TNF-α-stimulation, NDP52 associates with LUBAC through the HOIP subunit, but does not disturb its ubiquitin ligase activity, and has a modest suppressive effect on NF-κB activation by functioning as a component of TNF-α receptor signaling complex I. NDP52 also regulates the TNF-α-induced apoptotic pathway, but not doxorubicin-induced intrinsic apoptosis. A chemical inhibitor of LUBAC (HOIPIN-8) cancelled the increased activation of the NF-κB and IFN antiviral pathways, and enhanced apoptosis in NDP52-knockout and -knockdown HeLa cells. Upon Salmonella-infection, colocalization of Salmonella, LC3, and linear ubiquitin was detected in parental HeLa cells to induce xenophagy. Treatment with HOIPIN-8 disturbed the colocalization and facilitated Salmonella expansion. In contrast, HOIPIN-8 showed little effect on the colocalization of LC3 and Salmonella in NDP52-knockout cells, suggesting that NDP52 is a weak regulator in LUBAC-mediated xenophagy. These results indicate that the crosstalk between NDP52 and LUBAC regulates innate immune responses, apoptosis, and xenophagy.

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Section: Resultsmentioning

confidence: 99%

“…NDP52 is a multifunctional regulatory protein that predominantly works in selective autophagy ( 17 , 18 ). Although linear (de)ubiquitination is involved in the NDP52-mediated xenophagy of invading Salmonella ( 24 , 25 ), little is known about the crosstalk between NDP52 and LUBAC in innate immune responses.…”

Section: Discussionmentioning

confidence: 99%

Crosstalk Between NDP52 and LUBAC in Innate Immune Responses, Cell Death, and Xenophagy

et al. 2021

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“…In addition to binding myosin VI, T6BP/TAX1BP1 and CALCOCO2/NDP52 also bind each other and have been suggested to modulate cytokine signaling and membrane transport with actin filament organization and cell adhesion [ 47 ]. There are several recent studies on CALCOCO2/NDP52 that have revealed important molecular insights on its role as the recruiter of the early autophagic protein complexes to the cargo, initiating selective autophagy [ 48 – 50 ], and a recent review summarizes its role in microbial infections, including viruses [ 51 ]. CALCOCO2/NDP52 has a role in innate immunity through NFKB and type I IFN regulation, which can be another explanation for CSFV CALCOCO2/NDP52 targeting.…”

Section: Discussionmentioning

confidence: 99%

Autophagy receptors as viral targets

Ylä-Anttila

2021

Cell Mol Biol Lett

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Activation of autophagy is part of the innate immune response during viral infections. Autophagy involves the sequestration of endogenous or foreign components from the cytosol within double-membraned vesicles and the delivery of their content to the lysosomes for degradation. As part of innate immune responses, this autophagic elimination of foreign components is selective and requires specialized cargo receptors that function as links between a tagged foreign component and the autophagic machinery. Pathogens have evolved ways to evade their autophagic degradation to promote their replication, and recent research has shown autophagic receptors to be an important and perhaps previously overlooked target of viral autophagy inhibition. This is a brief summary of the recent progress in knowledge of virus-host interaction in the context of autophagy receptors.

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“… 18 , 40 , 41 A previous report has shown that NDP52, an autophagy receptor, links autophagy and the UPS. 42 Rapamycin-induced autophagy promotes cell survival in the presence of proteasome inhibitors in vivo and in vitro. 43 , 44 Proteasome inhibition activates autophagy, with p62 acting as a bridge.…”

Section: Discussionmentioning

confidence: 99%

Immunosubunit β5i Knockout Suppresses Neovascularization and Restores Autophagy in Retinal Neovascularization by Targeting ATG5 for Degradation

Zhao³

et al. 2020

Invest. Ophthalmol. Vis. Sci.

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The Role of Autophagy and Autophagy Receptor NDP52 in Microbial Infections

Cited by 15 publications

References 99 publications

Crosstalk Between NDP52 and LUBAC in Innate Immune Responses, Cell Death, and Xenophagy

Crosstalk Between NDP52 and LUBAC in Innate Immune Responses, Cell Death, and Xenophagy

Autophagy receptors as viral targets

Immunosubunit β5i Knockout Suppresses Neovascularization and Restores Autophagy in Retinal Neovascularization by Targeting ATG5 for Degradation

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