Equilibrative nucleoside transporter 3 depletion in β-cells impairs mitochondrial function and promotes apoptosis: Relationship to pigmented hypertrichotic dermatosis with insulin-dependent diabetes

Liu, Bo; Czajka, Anna; Malik, Afshan N.; Hussain, Khalid; Jones, Peter M.; Persaud, Shanta J.

doi:10.1016/j.bbadis.2015.07.002

Cited by 16 publications

(9 citation statements)

References 51 publications

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“…Its gene knockdown suppresses depolarization-evoked ATP release from cultured astrocytes [106]. However, ENT3 prefers nucleosides and nucleobases as substrates, which differs from the content of nucleotides stored in ATP-storing organelles, and is mainly localized in mitochondria [107,108]. These findings support the idea that ENT3 is not involved in the vesicular storage of nucleotides.…”

Section: Additional Vesicular Atp Transporter Candidatessupporting

confidence: 52%

Vesicular nucleotide transporter (VNUT): appearance of an actress on the stage of purinergic signaling

Moriyama

Hiasa

Sakamoto³

et al. 2017

Purinergic Signalling

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Vesicular storage of ATP is one of the processes initiating purinergic chemical transmission. Although an active transport mechanism was postulated to be involved in the processes, a transporter(s) responsible for the vesicular storage of ATP remained unidentified for some time. In 2008, SLC17A9, the last identified member of the solute carrier 17 type I inorganic phosphate transporter family, was found to encode the vesicular nucleotide transporter (VNUT) that is responsible for the vesicular storage of ATP. VNUT transports various nucleotides in a membrane potential-dependent fashion and is expressed in the various ATP-secreting cells. Mice with knockout of the VNUT gene lose vesicular storage and release of ATP from neurons and neuroendocrine cells, resulting in blockage of the initiation of purinergic chemical transmission. Thus, VNUT plays an essential role in the vesicular storage and release of ATP. The VNUT knockout mice exhibit resistance for neuropathic pain and a therapeutic effect against diabetes by way of increased insulin sensitivity. Thus, VNUT inhibitors and suppression of VNUT gene expression may be used for therapeutic purposes through suppression of purinergic chemical transmission. This review summarizes the studies to date on VNUT and discusses what we have learned about the relevance of vesicular ATP release as a potential drug target.

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Section: Additional Vesicular Atp Transporter Candidatessupporting

confidence: 52%

Vesicular nucleotide transporter (VNUT): appearance of an actress on the stage of purinergic signaling

Moriyama

Hiasa

Sakamoto³

et al. 2017

Purinergic Signalling

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“…SLC29A3 encodes a nucleoside transporter which plays a significant role in the cellular uptake of nucleosides and nucleobases. It was previously reported that many diseases were related to RAD51AP1 expression, including autoinflammatory diseases [ 46 ], H syndrome [ 47 ], insulin-dependent diabetes [ 48 ], pigmentary hypertrichosis, autoimmune insulin-dependent diabetes mellitus [ 49 ], and sclerosing bone dysplasias [ 50 ]. Meanwhile, MIMT1 is an MER1 repeat-containing imprinted transcript, which can undergo hypermethylation in the placenta of intrauterine growth-restricted fetuses in cattle [ 51 ], and truncation of exons 3 and 4 of the MIMT1 gene caused intrauterine growth restriction [ 52 ].…”

Section: Discussionmentioning

confidence: 99%

Identification of the Novel Methylated Genes’ Signature to Predict Prognosis in INRG High-Risk Neuroblastomas

Liu

2021

Journal of Oncology

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Background. Neuroblastomas are the most frequent extracranial pediatric solid tumors. The prognosis of children with high-risk neuroblastomas has remained poor in the past decade. A powerful signature is required to identify factors associated with prognosis and improved treatment selection. Here, we identified a strong methylation signature that favored the earlier diagnosis of neuroblastoma in patients. Methods. Gene methylation (GM) data of neuroblastoma patients from the Therapeutically Applicable Research to Generate Effective Treatments (TARGET) were analyzed using a multivariate Cox regression analysis (MCRA) and univariate Cox proportional hazards regression analysis (UCPHRA). Results. The methylated genes’ signature consisting of eight genes (NBEA, DDX28, TMED8, LOC151174, EFNB2, GHRHR, MIMT1, and SLC29A3) was selected. The signature divided patients into low- and high-risk categories, with statistically significant survival rates (median survival time: 25.08 vs. >128.80 months, log-rank test, P < 0.001 ) in the training group, and the validation of the signature’s risk stratification ability was carried out in the test group (log-rank test, P < 0.01 , median survival time: 30.48 vs. >120.36 months). The methylated genes’ signature was found to be an independent predictive factor for neuroblastoma by MCRA. Functional enrichment analysis suggested that these methylated genes were related to butanoate metabolism, beta-alanine metabolism, and glutamate metabolism, all playing different significant roles in the process of energy metabolism in neuroblastomas. Conclusions. The set of eight methylated genes could be used as a new predictive and prognostic signature for patients with INRG high-risk neuroblastomas, thus assisting in treatment, drug development, and predicting survival.

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“…Since 2014, 17 patients have been reported. 11,20,[23][24][25][26][27][28][29][30] Molho-Pessach et al 5 emphasized that the finding of several different mutations in a small geographic region implies that H syndrome may be rather common and underdiagnosed owing to the fact that many patients have a very mild clinical presentation. In our context, geographic endogamy is frequent in Tunisia, especially in rural areas where it could reach 90% and familial endogamy or interrelated marriages are profoundly rooted with an estimated rate of 30% of all kind of unions.…”

Section: Discussionmentioning

confidence: 99%

H syndrome: Clinical, histological and genetic investigation in Tunisian patients

Jaouadi

Zaouak

Sellami

et al. 2018

The Journal of Dermatology

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H syndrome is a rare autosomal recessive disorder with characteristic dermatological findings consisting of hyperpigmentation and hypertrichosis patches mainly located on the inner thighs and multisystemic involvement including hepatosplenomegaly, hearing loss, heart abnormalities and hypogonadism. The aim of this study was to conduct a clinical and genetic investigation in five unrelated Tunisian patients with suspected H syndrome. Hence, genetic analysis of the SLC29A3 gene was performed for four patients with a clinical diagnosis of H syndrome. We identified a novel frame-shift mutation in the SLC29A3 gene in a female patient with a severe clinical presentation. Furthermore, we report two mutations previously described, the p.R363Q mutation in a male patient and the p.P324L mutation in two patients of different age and sex. This paper extends the mutation spectrum of H syndrome by reporting a novel frame-shift mutation, the p.S15Pfs*86 in exon 2 of SLC29A3 gene and emphasizes the relevance of genetic testing for its considerable implications in early diagnosis and clinical management.

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Equilibrative nucleoside transporter 3 depletion in β-cells impairs mitochondrial function and promotes apoptosis: Relationship to pigmented hypertrichotic dermatosis with insulin-dependent diabetes

Cited by 16 publications

References 51 publications

Vesicular nucleotide transporter (VNUT): appearance of an actress on the stage of purinergic signaling

Vesicular nucleotide transporter (VNUT): appearance of an actress on the stage of purinergic signaling

Identification of the Novel Methylated Genes’ Signature to Predict Prognosis in INRG High-Risk Neuroblastomas

H syndrome: Clinical, histological and genetic investigation in Tunisian patients

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