The V-ATPase a3 Subunit: Structure, Function and Therapeutic Potential of an Essential Biomolecule in Osteoclastic Bone Resorption

Chu, Anh; Zirngibl, Ralph A; Manolson, Morris F.

doi:10.3390/ijms22136934

Cited by 22 publications

(20 citation statements)

References 180 publications

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“…V-ATPase containing an a3 isoform translocates to the plasma membrane, acidifying the extracellular space to promote bone resorption. Mutations in the T-cell immune regulator 1, ATPase H + transporting V0 subunit A3 (TCIRG1) gene encoding the a3 isoform are highly associated with osteoporosis [ 55 ]. These findings indicate that abnormal V-ATPase trafficking leads to inflammation-related diseases, such as osteoporosis.…”

Section: Regulation Of V-atpase Activitymentioning

confidence: 99%

The V-ATPases in cancer and cell death

et al. 2022

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Transmembrane ATPases are membrane-bound enzyme complexes and ion transporters that can be divided into F-, V-, and A-ATPases according to their structure. The V-ATPases, also known as H + -ATPases, are large multi-subunit protein complexes composed of a peripheral domain (V1) responsible for the hydrolysis of ATP and a membrane-integrated domain (V0) that transports protons across plasma membrane or organelle membrane. V-ATPases play a fundamental role in maintaining pH homeostasis through lysosomal acidification and are involved in modulating various physiological and pathological processes, such as macropinocytosis, autophagy, cell invasion, and cell death (e.g., apoptosis, anoikis, alkaliptosis, ferroptosis, and lysosome-dependent cell death). In addition to participating in embryonic development, V-ATPase pathways, when dysfunctional, are implicated in human diseases, such as neurodegenerative diseases, osteopetrosis, distal renal tubular acidosis, and cancer. In this review, we summarize the structure and regulation of isoforms of V-ATPase subunits and discuss their context-dependent roles in cancer biology and cell death. Updated knowledge about V-ATPases may enable us to design new anticancer drugs or strategies.

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Section: Regulation Of V-atpase Activitymentioning

confidence: 99%

The V-ATPases in cancer and cell death

et al. 2022

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“…A coding gene signature of subunits and chaperones of the V-ATPase was acquired from a previous study [ 14 ], including 14 genes of the V1 subunit (ATP6V1A, ATP6V1B1, ATP6V1B2, ATP6V1C1, ATP6V1C2, ATP6V1C3, ATP6V1D, ATP6V1E1, ATP6V1E2, ATP6V1F, ATP6V1G1, ATP6V1G2, ATP6V1G3 and ATP6V1H), 13 genes of the V0 subunit (ATP6V0A1, ATP6V0A2, TCIRG1, ATP6V0A4, ATP6V0C, ATP6V0B, ATP6V0D1, ATP6V0D2, ATP6V0E1, ATP6V0E2, RNASEK, ATP6AP1 and ATP6AP2) and three chaperone molecules (TMEM199, VMA21 and CCDC115). Transcriptome data of glioma patients were acquired from the Cancer Genome Atlas (TCGA) using the UCSC Xena browser (TCGA-GBMLGG dataset (n = 702), https://xenabrowser.net/datapages/ ) and the Chinese Glioma Genome Atlas (CGGA) database (CGGA-mRNA693 (n = 693), CGGA-mRNA325 (n = 325) and CGGA-mRNA301 (n = 301), http://www.cgga.org.cn/ ) and Gliovis platform (Rembrandt (n = 472) and Gravendeel (n = 284), http://gliovis.bioinfo.cnio.es ) [ 15–25 ].…”

Section: Methodsmentioning

confidence: 99%

Identification of a five-gene signature deriving from the vacuolar ATPase (V-ATPase) sub-classifies gliomas and decides prognoses and immune microenvironment alterations

Cui

Lei

et al. 2022

Cell Cycle

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Aberrant expression of coding genes of the V-ATPase subunits has been reported in glioma patients that can activate oncogenic pathways and result in worse prognosis. However, the predictive effect of a single gene is not specific or sensitive enough. In this study, by using a series of bioinformatics analyses, we identified five coding genes (ATP6V1C2, ATP6V1G2, TCIRG1, ATP6AP1 and ATP6AP2) of the V-ATPase that were related to glioma patient prognosis. Based on the expression of these genes, glioma patients were sub-classified into different prognosis clusters, of which C1 cluster performed better prognosis; however, C2 cluster showed more malignant phenotypes with oncogenic and immune-related pathway activation. The single-cell RNA-seq data revealed that ATP6AP1, ATP6AP2, ATP6V1G2 and TCIRG1 might be cell-type potential markers. Copy number variation and DNA promoter methylation potentially regulate these five gene expressions. A risk score model consisted of these five genes effectively predicted glioma prognosis and was fully validated by six independent datasets. The risk scores also showed a positive correlation with immune checkpoint expression. Importantly, glioma patients with high-risk scores presented resistance to traditional treatment. We also revealed that more inhibitory immune cells infiltration and higher rates of “non-response” to immune checkpoint blockade (ICB) treatment in the high-risk score group. In conclusion, our study identified a five-gene signature from the V-ATPase that could sub-classify gliomas into different phenotypes and their abnormal expression was regulated by distinct mechanisms and accompanied with immune microenvironment alterations potentially act as a biomarker for ICB treatment.

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“…The V 1 sector is a soluble complex with three catalytic A subunits, and the V o sector is a membrane-embedded complex with a proton pathway formed by the a subunit and the c-ring. [13][14][15][16][17][18] Similar to F-ATPase (ATP synthase), V-ATPase couples catalysis and proton transport through subunit rotation, which is called rotational catalysis. [16][17][18] The mechanism has been analyzed in detail using bacterial enzymes, and these studies have been covered elsewhere.…”

Section: Introductionmentioning

confidence: 99%

“…[19][20][21] Among the subunits composing mammalian V-ATPase, six subunits have cell-and/or organellespecific isoforms, resulting in diversity in isoform composition. [13][14][15][16][17][18] For example, the a subunit in the V o sector has four isoforms (a1, a2, a3, and a4). The a4 isoform is specifically expressed in kidney, while the other three isoforms are ubiquitously expressed, but localized in specific organelles.…”

Section: Introductionmentioning

confidence: 99%

V-ATPase a3 Subunit in Secretory Lysosome Trafficking in Osteoclasts

Nakanishi‐Matsui

Matsumoto

2022

Biological & Pharmaceutical Bulletin

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Vacuolar-type ATPase (V-ATPase) shares its structure and rotational catalysis with F-type ATPase (F-ATPase, ATP synthase). However, unlike subunits of F-ATPase, those of V-ATPase have tissue-and/or organelle-specific isoforms. Structural diversity of V-ATPase generated by different combinations of subunit isoforms enables it to play diverse physiological roles in mammalian cells. Among these various roles, this review focuses on the functions of lysosome-specific V-ATPase in bone resorption by osteoclasts. Lysosomes remain in the cytoplasm in most cell types, but in osteoclasts, secretory lysosomes move toward and fuse with the plasma membrane to secrete lysosomal enzymes, which is essential for bone resorption. Through this process, lysosomal V-ATPase harboring the a3 isoform of the a subunit is relocated to the plasma membrane, where it transports protons from the cytosol to the cell exterior to generate the acidic extracellular conditions required for secreted lysosomal enzymes. In addition to this role as a proton pump, we recently found that the lysosomal a3 subunit of V-ATPase is essential for anterograde trafficking of secretory lysosomes. Specifically, a3 interacts with Rab7, a member of the Rab guanosine 5ʹ-triphosphatase (GTPase) family that regulates organelle trafficking, and recruits it to the lysosomal membrane. These findings revealed the multifunctionality of lysosomal V-ATPase in osteoclasts; V-ATPase is responsible not only for the formation of the acidic environment by transporting protons, but also for intracellular trafficking of secretory lysosomes by recruiting organelle trafficking factors. Herein, we summarize the molecular mechanism underlying secretory lysosome trafficking in osteoclasts, and discuss the possible regulatory role of V-ATPase in organelle trafficking.

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The V-ATPase a3 Subunit: Structure, Function and Therapeutic Potential of an Essential Biomolecule in Osteoclastic Bone Resorption

Cited by 22 publications

References 180 publications

The V-ATPases in cancer and cell death

The V-ATPases in cancer and cell death

Identification of a five-gene signature deriving from the vacuolar ATPase (V-ATPase) sub-classifies gliomas and decides prognoses and immune microenvironment alterations

V-ATPase a3 Subunit in Secretory Lysosome Trafficking in Osteoclasts

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