MCOLN1 Promotes Proliferation and Predicts Poor Survival of Patients with Pancreatic Ductal Adenocarcinoma

Hu, Zhandong; Yan, Jun; Cao, Kai-Yue; Yin, Zhiqi; Xin, Wei-Wei; Zhang, Mingfang

doi:10.1155/2019/9436047

Cited by 23 publications

(31 citation statements)

References 34 publications

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“…In non-small-cell lung cancer, increased TRPML1 expression is observed at high tumor stages and is positively correlated with tumor proliferation, migration, and invasion [ 26 ]. Consistent with this finding, TRPML1 expression is also increased in pancreatic ductal adenocarcinoma (PDAC) patients and negatively correlates with patient overall survival and recurrence-free survival [ 27 ]. Since cancer cells aggressively augment protein synthesis machineries to stimulate cell proliferation, cancer cells experience elevated proteotoxic stress due to increased occurrences of translational infidelity and susceptibility to protein misfolding in the endoplasmic reticulum, potentially triggering cell death [ 28 , 29 ].…”

Section: Main Documentmentioning

confidence: 76%

TRPML1—Emerging Roles in Cancer

Yang

Zhai

Hiani

2020

Cells

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The mucolipin-1 (TRPML1) channel maintains lysosomal ionic homeostasis and regulates autophagic flux. Defects of TRPML1 lead to lysosomal storage diseases and neurodegeneration. In this report, we discuss emerging evidence pertaining to differential regulation of TRPML1 signaling pathways in cancer progression with the goal of leveraging the oncogenic potential of TRPML1 to inspire therapeutic interventions.

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Section: Main Documentmentioning

confidence: 76%

TRPML1—Emerging Roles in Cancer

Yang

Zhai

Hiani

2020

Cells

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“…Yin et al [ 122 ] found that the expression of TRPML1 increases along with the progression of human nonsmall-cell lung cancer (NSCLC). Similarly, by evaluating the expression levels of TRPML1 in tumor tissues from 82 pancreatic ductal adenocarcinoma (PDAC) patients, Hu et al found that a higher TRPML1 expression level is associated with the poor clinical characteristics of these PDAC patients [ 123 ]. Compared with patients with low TRPML1 expression, patients with high TRPML1 expression have significantly lower overall survival.…”

Section: The Lysosomal Ca 2+ Channel Trpmls In mentioning

confidence: 99%

“…Compared with patients with low TRPML1 expression, patients with high TRPML1 expression have significantly lower overall survival. A role of TRPML1 in PDAC progression is further confirmed by using a cell model showing that the proliferation of PDAC cells is dramatically blocked by TRPML1 depletion, and by using a mouse model showing that TRPML1 is required for the formation and growth of PDAC tumors [ 123 ]. Collectively, these studies suggest that TRPML1 is often upregulated in cancer cells to promote tumorigenesis.…”

Section: The Lysosomal Ca 2+ Channel Trpmls In mentioning

confidence: 99%

Endolysosomal TRPMLs in Cancer

Dong

2021

Biomolecules

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Lysosomes, the degradative endpoints and sophisticated cellular signaling hubs, are emerging as intracellular Ca2+ stores that govern multiple cellular processes. Dys-homeostasis of lysosomal Ca2+ is intimately associated with a variety of human diseases including cancer. Recent studies have suggested that the Ca2+-permeable channels Transient Receptor Potential (TRP) Mucolipins (TRPMLs, TRPML1-3) integrate multiple processes of cell growth, division and metabolism. Dysregulation of TRPMLs activity has been implicated in cancer development. In this review, we provide a summary of the latest development of TRPMLs in cancer. The expression of TRPMLs in cancer, TRPMLs in cancer cell nutrient sensing, TRPMLs-mediated lysosomal exocytosis in cancer development, TRPMLs in TFEB-mediated gene transcription of cancer cells, TRPMLs in bacteria-related cancer development and TRPMLs-regulated antitumor immunity are discussed. We hope to guide readers toward a more in-depth discussion of the importance of lysosomal TRPMLs in cancer progression and other human diseases.

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“…While insufficient endolysosomal function is associated with inborn errors of metabolism, lysosomal storage, and degenerative diseases, increased biogenesis of these organelles is a recurring theme in cancers (Davidson and Vander Heiden, 2017). Several studies have described roles for the endolysosomal cation channel, TRPML1, in different malignancies (Hu et al, 2019;Kasitinon et al, 2019;Xu et al, 2019;Yin et al, 2019). A common theme in these studies is that TRPML1 is necessary for malignancy promoting signaling cascades involving RAS-MAPK and mTORC1.…”

Section: Introductionmentioning

confidence: 99%

“…Since inhibition of TRPML1 arrests proliferation or induces cell death in cancers with elevated expression of the CLEAR network genes (Hu et al, 2019;Jung and Venkatachalam, 2019;, tumors with hyperactivated TFEB/TFE3/MITF signaling are addicted to TRPML1.…”

Section: Introductionmentioning

confidence: 99%

ElevatedMCOLN1Expression in p53-Deficient Bladder Cancer is Necessary for Oncogene-Induced Cell proliferation, Inflammation, and Invasion

Jung

Han

Luan

et al. 2020

Preprint

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SummaryInhibition of the endolysosomal cation channel, TRPML1, which is encoded by MCOLN1, deters the proliferation of cancer cells with augmented TFEB activity. Here, we report that the tumor suppressor, p53, antagonizes TFEB-driven MCOLN1 expression in bladder cancer. Not only was the constitutive loss of p53 in bladder cancer cells associated with higher MCOLN1 mRNA, knockdown of TP53 in lines with wild type alleles of the tumor suppressor increased MCOLN1 expression. Elevated TRPML1 abundance in p53-deficient cancer cells, although not sufficient for bolstering proliferation, was necessary for the effects of oncogenic HRAS on cell division, cytokine production, and invasion. These data demonstrate that hyperactivation of the TFEB– MCOLN1 transcriptional axis in urothelial cells lacking p53 permits tumorigenesis stemming from HRAS mutations. Furthermore, the insight that loss of p53 predicts addiction to TRPML1 informs an actionable therapeutic strategy for bladder cancer.

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MCOLN1 Promotes Proliferation and Predicts Poor Survival of Patients with Pancreatic Ductal Adenocarcinoma

Cited by 23 publications

References 34 publications

TRPML1—Emerging Roles in Cancer

TRPML1—Emerging Roles in Cancer

Endolysosomal TRPMLs in Cancer

ElevatedMCOLN1Expression in p53-Deficient Bladder Cancer is Necessary for Oncogene-Induced Cell proliferation, Inflammation, and Invasion

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