Autophagy suppresses progression of K-ras-induced lung tumors to oncocytomas and maintains lipid homeostasis

Guo, Jessie Yanxiang; Karsli-Uzunbas, Gizem; Mathew, Robin; Aisner, Seena C.; Kamphorst, Jurre J.; Strohecker, Anne M.; Chen, Guanghua; Price, Sandy M.; Lu, Wenyun; Teng, Xin; Snyder, Eric L.; Santanam, Urmila; DiPaola, Robert S.; Jacks, Tyler; Rabinowitz, Joshua D.; White, Eileen

doi:10.1101/gad.219642.113

Cited by 535 publications

(614 citation statements)

References 35 publications

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“…26 In a separate study, it was also demonstrated that the loss of Atg5 or Atg7 could also prevent the development of high-grade pancreatic neoplastic legions induced by K-ras, and the pancreatic tumor growth could be restored if the expression of p53 was also abolished. 27 These recent findings together with ours indicate that autophagy is required for tumor progression for at least three different tumor types and that the deletion of p53 can partially restore tumorigenesis when autophagy is impaired.…”

Section: Discussionmentioning

confidence: 97%

Autophagy inhibits oxidative stress and tumor suppressors to exert its dual effect on hepatocarcinogenesis

et al. 2014

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The role of autophagy in carcinogenesis is controversial and apparently complex. By using mice with hepatocyte-specific knockout of Atg5, a gene essential for autophagy, we longitudinally studied the role of autophagy in hepatocarcinogenesis. We found that impairing autophagy in hepatocytes would induce oxidative stress and DNA damage, followed by the initiation of hepatocarcinogenesis, which could be suppressed by the antioxidant N-acetylcysteine. Interestingly, these mice developed only benign tumors with no hepatocellular carcinoma (HCC), even after the treatment with diethylnitrosamine, which induced HCC in wild-type mice. The inability of mice to develop HCC when autophagy was impaired was associated with the induction of multiple tumor suppressors including p53. Further analysis indicated that the induction of p53 was associated with the DNA-damage response. Tumorigenesis studies using an established liver tumor cell line confirmed a positive role of autophagy in tumorigenesis and a negative role of p53 in this process when autophagy was impaired. Our studies thus demonstrate that autophagy is required to maintain healthy mitochondria and to reduce oxidative stress and DNA damage to prevent the initiation of hepatocarcinogenesis. However, once hepatocarcinogenesis has been initiated, its presence is also required to suppress the expression of tumor suppressors to promote the development of HCC. Autophagy (i.e., macroautophagy) is important for cells to remove protein aggregates and damaged organelles. Its dysfunction can cause a variety of diseases including cancers. 1,2 However, its role in carcinogenesis is apparently complex, as it has been shown in different reports to positively or negatively regulate carcinogenesis. 3,4 Autophagy apparently can function as a tumor suppressor, as the gene encoding Beclin-1, a component of the phosphatidylinositol-3-kinase class III (PI3KC3) complex that is essential for the initiation of autophagy, is often monoallelically deleted or mutated in breast, ovarian and prostate cancers. 5 Frameshift mutations in Atg2B, Atg5, Atg9B and Atg12 autophagy genes are also often found in gastric and colorectal cancers with microsatellite instability. 6 The tumor suppressor role of autophagy is further supported by the studies using mouse models. It has been shown that the monoallelic deletion of the Beclin-1 gene in mice induced tumor lesions in various tissues, 7 Atg4C-knockout (KO) mice had increased susceptibility to carcinogens for the development of fibrosarcomas 8 and the systemic mosaic KO of Atg5 and the liver-specific KO of Atg7 in mice led to the development of benign liver adenomas. 9,10 Autophagy has also been shown to promote tumor growth. It has been shown that autophagy can enhance the survival of tumor cells in the hypoxic regions of solid tumors. 11 It has also been shown that in cells expressing oncogenic Ras, autophagy is required to promote tumorigenesis by maintaining oxidative metabolism or facilitating glycolysis. 12,13 Moreover, it has also been demonstrate...

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Section: Discussionmentioning

confidence: 97%

Autophagy inhibits oxidative stress and tumor suppressors to exert its dual effect on hepatocarcinogenesis

et al. 2014

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“…26 The core autophagy machinery may be protected from alteration in some human cancers, an idea supported by recent studies in murine models of lung cancer that find autophagy to be essential for tumor progression. 27,28 Importantly, we found that clustering abundance profiles of AA genes stratified patient OS in 3 of 9 cancer types and grouped patients with similar pathophysiology together, linking the differential expression of autophagy regulators and interactors to clinical features known to influence patient outcome. This suggests that clinically relevant differential pathway activities exist between …”

Section: Discussionmentioning

confidence: 97%

“…72 Autophagy has been shown to support tumorigenesis in lung cancer, particularly in KRAS-driven lung cancer cell lines and animal models that may be addicted to high levels of autophagy, 73,74 and autophagy inactivation in KRasdriven mouse models of lung cancer impairs cell growth, proliferation, and tumor progression. 27,28 We stratified gene expression of all 211 AA genes in both LUAD and LUSC by known recurrent somatic disease-specific alterations, including EGFR and KRAS alterations, and did not find differences in core gene expression between altered and wild-type patients; however, LUSC patients with EGFR amplification had increased mRNA levels of NFE2L2 (median FC > 2; Table S5). Both overactive and impaired autophagy are hypothesized to support oncogenic NFE2L2 activity in cancer, 75 through increased degradation of the NFE2L2 sequestering protein KEAP1 51 or through reduced degradation of KEAP1 binding protein SQSTM1/p62, 76 respectively.…”

Section: Clear Cell Renal Carcinomamentioning

confidence: 99%

“…38,39 BNIP3's contribution to tumorigenesis has yet to be linked to its role in mitophagy; however, the fact that increased levels of BNIP3 are associated with more aggressive disease suggests that a function in tumor cell survival via autophagy or mitophagy is a more likely mechanistic scenario than a role in cell death, in contexts of BNIP3 overexpression. Autophagy has documented roles in KRAS-driven lung 27,28 and pancreatic 40,41 cancer progression, and overactive RAS has been shown to upregulate BNIP3. 42 Further investigation of autophagy status in RAS-driven tumors with BNIP3 overexpression may reveal a mechanistic link between BNIP3 and tumor cell survival.…”

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confidence: 99%

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Cross-cancer profiling of molecular alterations within the human autophagy interaction network

et al. 2015

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Aberrant activation or disruption of autophagy promotes tumorigenesis in various preclinical models of cancer, but whether the autophagy pathway is a target for recurrent molecular alteration in human cancer patient samples is unknown. To address this outstanding question, we surveyed 211 human autophagy-associated genes for tumorrelated alterations to DNA sequence and RNA expression levels and examined their association with patient survival outcomes in multiple cancer types with sequence data from The Cancer Genome Atlas consortium. We found 3 (RB1CC1/FIP200, ULK4, WDR45/WIPI4) and one (ATG7) core autophagy genes to be under positive selection for somatic mutations in endometrial carcinoma and clear cell renal carcinoma, respectively, while 29 autophagy regulators and pathway interactors, including previously identified KEAP1, NFE2L2, and MTOR, were significantly mutated in 6 of the 11 cancer types examined. Gene expression analyses revealed that GABARAPL1 and MAP1LC3C/LC3C transcripts were less abundant in breast cancer and non-small cell lung cancers than in matched normal tissue controls; ATG4D transcripts were increased in lung squamous cell carcinoma, as were ATG16L2 transcripts in kidney cancer. Unsupervised clustering of autophagy-associated mRNA levels in tumors stratified patient overall survival in 3 of 9 cancer types (acute myeloid leukemia, clear cell renal carcinoma, and head and neck cancer). These analyses provide the first comprehensive resource of recurrently altered autophagy-associated genes in human tumors, and highlight cancer types and subtypes where perturbed autophagy may be relevant to patient overall survival.

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“…It has been suggested to hold a tumour suppressive function during early tumourigenesis, [20][21][22][23][24][25][26][27] whereas it can also sustain cancer progression. [28][29][30][31][32][33][34][35][36] Increased levels of basal autophagy have been found in a variety of cancer tissues including colorectal cancer (CRC), where autophagy supports tumour growth and confers tumour aggressiveness. 31 Autophagy is inhibited by oncogenic tyrosine kinases (OncTKs) and receptor tyrosine kinases (RTKs) via activation of the PI3K/AKT/mTORC1 and RAS/MAPK signalling.…”

Section: Introductionmentioning

confidence: 99%

mTORC1-independent autophagy regulates receptor tyrosine kinase phosphorylation in colorectal cancer cells via an mTORC2-mediated mechanism

et al. 2017

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The intracellular autophagic degradative pathway can play tumour suppressive or tumour promoting roles depending on the stage of tumour development. Upon starvation or targeting of oncogenic receptor tyrosine kinases (RTKs), autophagy is activated due to inhibition of PI3K/AKT/mTORC1 signalling pathway and promotes survival, suggesting that autophagy is a relevant therapeutic target in these settings.

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Autophagy suppresses progression of K-ras-induced lung tumors to oncocytomas and maintains lipid homeostasis

Cited by 535 publications

References 35 publications

Autophagy inhibits oxidative stress and tumor suppressors to exert its dual effect on hepatocarcinogenesis

Autophagy inhibits oxidative stress and tumor suppressors to exert its dual effect on hepatocarcinogenesis

Cross-cancer profiling of molecular alterations within the human autophagy interaction network

mTORC1-independent autophagy regulates receptor tyrosine kinase phosphorylation in colorectal cancer cells via an mTORC2-mediated mechanism

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