Autophagy gene expression profiling identifies a defective microtubule-associated protein light chain 3A mutant in cancer

Costa, Joana R.; Prak, Krisna; Aldous, Sarah; Gewinner, Christina; Ketteler, Robin

doi:10.18632/oncotarget.9754

Cited by 18 publications

(22 citation statements)

References 44 publications

(48 reference statements)

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“…Statistical significance determined by the two-tailed unpaired Student's t-test, using Holm-Sidak correction, *P < 0.05; **P < 0.01. mutations in autophagy genes in human cancer patient samples, the most frequent gene mutations are in autophagy regulators and pathway interactors, rather than mutations in the core machinery of autophagy [22,23]. Among the few reports on the latter group is a cancer-associated mutation in MAP1LC3A [24], which results in the protein's reduced cleavage by ATG4B and reduced autophagy levels. Our computational analysis shown here confirmed that mutations in core-machinery autophagy genes are indeed rare in different types of cancer.…”

Section: Discussionmentioning

confidence: 99%

A cancer associated somatic mutation in LC3B attenuates its binding to E1-like ATG7 protein and subsequent lipidation

et al. 2018

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Macroautophagy/autophagy is a conserved catabolic process that maintains cellular homeostasis under basal growth and stress conditions. In cancer, autophagy can either prevent or promote tumor growth, at early or advanced stages, respectively. We screened public databases to identify autophagy-related somatic mutations in cancer, using a computational approach to identify cancer mutational target sites, employing exact statistics. The top significant hit was a missense mutation (Y113C) in the MAP1LC3B/ LC3B (microtubule associated protein 1 light chain 3 beta) protein, which occurred at a significant frequency in cancer, and was detected in early stages in primary tumors of patients with known tumor lineage. The mutation reduced the formation of GFP-LC3B puncta and attenuated LC3B lipidation during Torin1-induced autophagy. Its effect on the direct physical interaction of LC3B with each of the 4 proteins that control its maturation or lipidation was tested by applying a protein-fragment complementation assay and co-immunoprecipitation experiments. Interactions with ATG4A and ATG4B proteases were reduced, yet without perturbing the cleavage of mutant LC3B. Most importantly, the mutation significantly reduced the interaction with the E1-like enzyme ATG7, but not the direct interaction with the E2-like enzyme ATG3, suggesting a selective perturbation in the binding of LC3B to some of its partner proteins. Structure analysis and molecular dynamics simulations of LC3B protein and its mutant suggest that the mutation changes the conformation of a loop that has several contact sites with ATG4B and the ATG7 homodimer. We suggest that this loss-of-function mutation, which attenuates autophagy, may promote early stages of cancer development. ARTICLE HISTORY

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Section: Discussionmentioning

confidence: 99%

A cancer associated somatic mutation in LC3B attenuates its binding to E1-like ATG7 protein and subsequent lipidation

et al. 2018

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“…We then searched in literature for experimental data that could validate our predictions, and we found results in agreement with the functional impact for mutations at R70, D19, G120, and K49, supporting our results. Mutations at R70 showed no accumulation of the pro-forms for LC3B (Liu et al, 2013), slower kinetics for Atg4B-mediated cleavage (Costa et al, 2016) and reduced binding for more that 20 interactors (Behrends et al, 2010;Kraft et al, 2014;Olsvik et al, 2015). G120 is fundamental for a proper C-terminal cleavage, which is impaired when this glycine is mutated to alanine (Tanida et al, 2004) and also G120 substitution with alanine has been shown to impair the binding of lamin B1 with LC3B (Dou et al, 2015).…”

Section: Classification and Impact Of Lc3b Missense Mutationsmentioning

confidence: 99%

The conformational and mutational landscape of the ubiquitin-like marker for the autophagosome formation in cancer

Fas

Kumar

Sora

et al. 2019

Preprint

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Autophagy is a cellular process to recycle damaged cellular components and its modulation can be exploited for disease treatments. A key autophagy player is a ubiquitin-like protein, LC3B. Compelling evidence attests the role of autophagy and LC3B in different cancer types. Many LC3B structures have been solved, but a comprehensive study, including dynamics, has not been yet undertaken. To address this knowledge gap, we assessed ten physical models for molecular dynamics for their capabilities to describe the structural ensemble of LC3B in solution using different metrics and comparison with NMR data. With the resulting LC3B ensembles, we characterized the impact of 26 missense mutations from Pan-Cancer studies with different approaches. Our findings shed light on driver or neutral mutations in LC3B, providing an atlas of its modifications in cancer. Our framework could be used to assess the pathogenicity of mutations by accounting for the different aspects of protein structure and function altered by mutational events.

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“…Instead, Met/LC3C complex formation requires both the LC3C C-terminal tail and residue R76 located within the ubiquitin-like domain of LC3C, and LC3C mutants lacking either of these cannot restore autophagy-dependent Met loss in LC3Cdepleted cells. Although LC3C interactions involving R76 have not previously been explored, mutations at this residue occur in human cancers (Costa et al, 2016). Although R76 is conserved in hATG8 proteins and large-scale proteomics analysis of the autophagy network identified that a portion of LC3B interactions are dependent on this residue (Behrends et al, 2010), LC3B does not engage with Met, highlighting that this residue alone is not sufficient.…”

Section: (F) Collagen Invasion Assays Performed As In (E) On Control mentioning

confidence: 99%

LC3C-Mediated Autophagy Selectively Regulates the Met RTK and HGF-Stimulated Migration and Invasion

et al. 2019

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The Met/hepatocyte growth factor (HGF) receptor tyrosine kinase (RTK) is deregulated in many cancers and is a recognized target for cancer therapies. Following HGF stimulation, the signaling output of Met is tightly controlled by receptor internalization and sorting for degradation or recycling. Here, we uncover a role for autophagy in selective degradation of Met and regulation of Met-dependent cell migration and invasion. Met engagement with the autophagic pathway is dependent on complex formation with the mammalian ATG8 family member MAP1LC3C. LC3C deletion abrogates Met entry into the autophagy-dependent degradative pathway, allowing identification of LC3C domains required for rescue. Cancer cells with low LC3C levels show enhanced Met stability, signaling, and cell invasion. These findings provide mechanistic insight into RTK recruitment to autophagosomes and establish distinct roles for ATG8 proteins in this process, supporting that differential expression of ATG8 proteins can shape the functional consequences of autophagy in cancer development and progression.

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Autophagy gene expression profiling identifies a defective microtubule-associated protein light chain 3A mutant in cancer

Cited by 18 publications

References 44 publications

A cancer associated somatic mutation in LC3B attenuates its binding to E1-like ATG7 protein and subsequent lipidation

A cancer associated somatic mutation in LC3B attenuates its binding to E1-like ATG7 protein and subsequent lipidation

The conformational and mutational landscape of the ubiquitin-like marker for the autophagosome formation in cancer

LC3C-Mediated Autophagy Selectively Regulates the Met RTK and HGF-Stimulated Migration and Invasion

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