Robust lysosomal calcium signaling through channel TRPML1 is impaired by lysosomal lipid accumulation

Gómez, Néstor; Lu, Wennan; Lim, Jason; Kiselyov, Kirill; Campagno, Keith E.; Grishchuk, Yulia; Slaugenhaupt, Susan A.; Pfeffer, Bruce A.; Fliesler, Steven J.; Mitchell, Claire H.

doi:10.1096/fj.201700220rr

Cited by 36 publications

(37 citation statements)

References 68 publications

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“…Next, we determined whether deletion of Rgs12 also affected Ca 2+ release from ER. To achieve that, cells were treated with 1µM TG to inhibit SERCA and unmask an endogenous leak for Ca 2+ . Similar to Ca 2+ influx, elevating amplitude of ER Ca 2+ release in Rgs12 d/d cells decreased dramatically (Fig.…”

Section: Resultsmentioning

confidence: 99%

“…Measurements of Ca 2+ oscillation were performed as described with slight modification . OPCs after Ad‐Null or Ad‐Cre infection were reseeded at a density of 2 × 10 5 cells/35‐mm dish and induced with OS medium for 3 days.…”

Section: Methodsmentioning

confidence: 99%

“…Change of intracellular Ca 2+ concentration was accessed and recorded for 45 min as mentioned in the first paragraph of section Ca 2+ imaging. Once the cells reached a stable baseline level of cytosolic Ca 2+ , the Ca 2+ ‐free ISO was exchanged for a Ca 2+ ‐free ISO containing 1µM TG (Sigma‐Aldrich) to trigger Ca 2+ release from the ER, a normal ISO containing 1.3mM CaCl 2 to induce extracellular Ca 2+ influx, or a normal ISO containing 10µM Bay K8644 (Sigma) to induce L‐type Ca 2+ channel amplified influx . Changes of intracellular Ca 2+ intensity were normalized by the initial Ca 2+ level of cell itself.…”

Section: Methodsmentioning

confidence: 99%

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Regulator of G Protein Signaling Protein 12 (Rgs12) Controls Mouse Osteoblast Differentiation via Calcium Channel/Oscillation and Gαi-ERK Signaling

Liu

Gilmore

et al. 2018

Journal of Bone and Mineral Research

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Bone homeostasis intimately relies on the balance between osteoblasts (OBs) and osteoclasts (OCs). Our previous studies have revealed that regulator of G protein signaling protein 12 (Rgs12), the largest protein in the Rgs super family, is essential for osteoclastogenesis from hematopoietic cells and OC precursors. However, how Rgs12 regulates OB differentiation and function is still unknown. To understand that, we generated an OB‐targeted Rgs12 conditional knockout (CKO) mice model by crossing Rgs12fl/fl mice with Osterix (Osx)‐Cre transgenic mice. We found that Rgs12 was highly expressed in both OB precursor cells (OPCs) and OBs of wild‐type (WT) mice, and gradually increased during OB differentiation, whereas Rgs12‐CKO mice (OsxCre/+; Rgs12fl/fl) exhibited a dramatic decrease in both trabecular and cortical bone mass, with reduced numbers of OBs and increased apoptotic cell population. Loss of Rgs12 in OPCs in vitro significantly inhibited OB differentiation and the expression of OB marker genes, resulting in suppression of OB maturation and mineralization. Further mechanism study showed that deletion of Rgs12 in OPCs significantly inhibited guanosine triphosphatase (GTPase) activity and cyclic adenosine monophosphate (cAMP) level, and impaired Calcium (Ca2+) oscillations via restraints of major Ca2+ entry sources (extracellular Ca2+ influx and intracellular Ca2+ release from endoplasmic reticulum), partially contributed by the blockage of L‐type Ca2+ channel mediated Ca2+ influx. Downstream mediator extracellular signal‐related protein kinase (ERK) was found inactive in OBs of OsxCre/+; Rgs12fl/fl mice and in OPCs after Rgs12 deletion, whereas application of pertussis toxin (PTX) or overexpression of Rgs12 could rescue the defective OB differentiation via restoration of ERK phosphorylation. Our findings reveal that Rgs12 is an important regulator during osteogenesis and highlight Rgs12 as a potential therapeutic target for bone disorders. © 2018 American Society for Bone and Mineral Research.

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Section: Resultsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

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Regulator of G Protein Signaling Protein 12 (Rgs12) Controls Mouse Osteoblast Differentiation via Calcium Channel/Oscillation and Gαi-ERK Signaling

Liu

Gilmore

et al. 2018

Journal of Bone and Mineral Research

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“…Furthermore, application of ML-SI1 significantly attenuated the proliferation of HN31 and T24 cells but not HT1197 or the cells that stably express HRAS shRNA (Figs 3C and EV2E and F). The PIKfyve inhibitor, YM201636, which inhibits PI(3,5)P 2 synthesis and TRPML1 activation [34,35], also diminished the proliferation of UM-SCC-22A-HRAS G12V and HN31 cells ( Fig EV2G). However, proliferation of cells that do not express oncogenic HRAS was not affected by YM201636 ( Fig EV2G).…”

Section: Trpml1 Is Required For the Proliferation Of Cancer Cells Expmentioning

confidence: 90%

HRAS‐driven cancer cells are vulnerable to TRPML1 inhibition

et al. 2019

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By serving as intermediaries between cellular metabolism and the bioenergetic demands of proliferation, endolysosomes allow cancer cells to thrive under normally detrimental conditions. Here, we show that an endolysosomal TRP channel, TRPML1, is necessary for the proliferation of cancer cells that bear activating mutations in HRAS. Expression of MCOLN1, which encodes TRPML1, is significantly elevated in HRAS‐positive tumors and inversely correlated with patient prognosis. Concordantly, MCOLN1 knockdown or TRPML1 inhibition selectively reduces the proliferation of cancer cells that express oncogenic, but not wild‐type, HRAS. Mechanistically, TRPML1 maintains oncogenic HRAS in signaling‐competent nanoclusters at the plasma membrane by mediating cholesterol de‐esterification and transport. TRPML1 inhibition disrupts the distribution and levels of cholesterol and thereby attenuates HRAS nanoclustering and plasma membrane abundance, ERK phosphorylation, and cell proliferation. These findings reveal a selective vulnerability of HRAS‐driven cancers to TRPML1 inhibition, which may be leveraged as an actionable therapeutic strategy.

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“…[45][46][47] The pathophysiological roles of FAIM2 in the nervous system would be of interest. Other molecules may substitute FAIM2 function in cells not expressing FAIM2.…”

Section: Discussionmentioning

confidence: 99%

Fas‐apoptotic inhibitory molecule 2 localizes to the lysosome and facilitates autophagosome‐lysosome fusion through the LC3 interaction region motif–dependent interaction with LC3

et al. 2019

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Abbreviations: BafA1, bafilomycin A1; BI-1, bax inhibitor-1; CASP, caspase; ER, endoplasmic reticulum; FAIM2, Fas-apoptotic inhibitory molecule 2; GABARAP, GABA type A receptor-associated protein; IDPR, intrinsically disordered protein region; LIR, LC3-interacting region; MAP1LC3B, microtubuleassociated protein 1 light chain 3 beta; MTOR, mammalian target of rapamycin; shRNA, small hairpin RNA; STX17, syntaxin 17; TMBIM, transmembrane BAX inhibitor motif containing. AbstractFas-apoptotic inhibitory molecule 2 (FAIM2) is a member of the transmembrane BAX inhibitor motif-containing (TMBIM) family. TMBIM family is comprised of six anti-apoptotic proteins that suppress cell death by regulating endoplasmic reticulum Ca 2+ homeostasis. Recent studies have implicated two TMBIM proteins, GRINA and BAX Inhibitor-1, in mediating cytoprotection via autophagy. However, whether FAIM2 plays a role in autophagy has been unknown. Here we show that FAIM2 localizes to the lysosomes at basal state and facilitates autophagy through interaction with microtubule-associated protein 1 light chain 3 proteins in human neuroblastoma SH-SY5Y cells. FAIM2 overexpression increased autophagy flux, while autophagy flux was impaired in shRNA-mediated knockdown (shFAIM2) cells, and the impairment was more evident in the presence of rapamycin. In shFAIM2 cells, autophagosome maturation through fusion with lysosomes was impaired, leading to accumulation of autophagosomes. A functional LC3-interacting region motif within FAIM2 was essential for the interaction with LC3 and rescue of autophagy flux in shFAIM2 cells while LC3-binding property of FAIM2 was dispensable for the antiapoptotic function in response to Fas receptor-mediated apoptosis. Suppression of autophagosome maturation was also observed in a null mutant of Caenorhabditis elegans lacking xbx-6, the ortholog of FAIM2. Our study suggests that FAIM2 is a novel regulator of autophagy mediating autophagosome maturation through the interaction with LC3.

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Robust lysosomal calcium signaling through channel TRPML1 is impaired by lysosomal lipid accumulation

Cited by 36 publications

References 68 publications

Regulator of G Protein Signaling Protein 12 (Rgs12) Controls Mouse Osteoblast Differentiation via Calcium Channel/Oscillation and Gαi-ERK Signaling

Regulator of G Protein Signaling Protein 12 (Rgs12) Controls Mouse Osteoblast Differentiation via Calcium Channel/Oscillation and Gαi-ERK Signaling

HRAS‐driven cancer cells are vulnerable to TRPML1 inhibition

Fas‐apoptotic inhibitory molecule 2 localizes to the lysosome and facilitates autophagosome‐lysosome fusion through the LC3 interaction region motif–dependent interaction with LC3

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