Wild‐type p53 regulates <scp>OTOP</scp>2 transcription through <scp>DNA</scp> loop alteration of the promoter in colorectal cancer

Qu, Huajun; Su, Yi; Yu, Lianzhi; Zhao, Hongchao; Xin, Chunxia

doi:10.1002/2211-5463.12554

Cited by 14 publications

(10 citation statements)

References 18 publications

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“…Interestingly, several genes whose precise molecular interactions are yet to be completely understood, are among the most highly expressed genes in both proximal and distal tumors including OTOP2 (controlled by wild-type TP53) [30], OTOP3, PYY and PPIAL4; and many with limited supporting evidence, might serve as interesting candidates for future research in colon cancers ( Supplementary Table S7). Additionally, several genes discussed herein are regulated across all stages further highlighting their role in the evolution and maintenance of tumors over time, in a side-independent manner (Fig.…”

Section: A Common Program Of Tumorigenesis Exists Between Right and Lmentioning

confidence: 99%

Right and left-sided colon cancers - specificity of molecular mechanisms in tumorigenesis and progression

et al. 2020

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Background: Given the differences in embryonic origin, vascular and nervous supplies, microbiotic burden, and main physiological functions of left and right colons, tumor location is increasingly suggested to dictate tumor behavior affecting pathology, progression and prognosis. Right-sided colon cancers arise in the cecum, ascending colon, hepatic flexure and/or transverse colon, while left-sided colon cancers arise in the splenic flexure, descending, and/or sigmoid colon. In contrast to prior reports, we attempt to delineate programs of tumorigenesis independently for each side. Methods: Four hundred and eleven samples were extracted from The Cancer Genome Atlas-COAD cohort, based on a conservative sample inclusion criterion. Each side was independently analyzed with respect to their respective normal tissue, at the level of transcription, post-transcription, miRNA control and methylation in both a stage specific and stage-agnostic manner. Results: Our results indicate a suppression of enzymes involved in various stages of carcinogen breakdown including CYP2C8, CYP4F12, GSTA1, and UGT1A within right colon tumors. This implies its reduced capacity to detoxify carcinogens, contributing to a genotoxic tumor environment, and subsequently a more aggressive phenotype. Additionally, we highlight a crucial nexus between calcium homeostasis (sensing, mobilization and absorption) and immune/GPCR signaling within left-sided tumors, possibly contributing to its reduced proliferative and metastatic potential. Interestingly, two genes SLC6A4 and HOXB13 show opposing regulatory trends within right and left tumors. Post-transcriptional regulation mediated by both RNA-binding proteins (e.g. NKRF (in left) and MSI2 (in right)) and miRNAs (e.g. miR-29a (in left); miR-155, miR181-d, miR-576 and miR23a (in right)) appear to exhibit side-specificity in control of their target transcripts and is pronounced in right colon tumors. Additionally, methylation results depict location-specific differences, with increased hypomethylation in open seas within left tumors, and increased hypermethylation of CpG islands within right tumors. Conclusions: Differences in molecular mechanisms captured here highlight distinctions in tumorigenesis and progression between left and right colon tumors, which will serve as the basis for future studies, influencing the efficacies of existing and future diagnostic, prognostic and therapeutic interventions.

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Section: A Common Program Of Tumorigenesis Exists Between Right and Lmentioning

confidence: 99%

Right and left-sided colon cancers - specificity of molecular mechanisms in tumorigenesis and progression

et al. 2020

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“…The founding member of the OTOP family, mOTOP1, was identified as the product of a gene mutated in a murine vestibular disorder ( Hurle et al, 2003 ; Hughes et al, 2004 ) and was subsequently shown to form a proton channel that functions as a receptor for sour taste in vertebrates ( Tu et al, 2018 ; Teng et al, 2019 ; Zhang et al, 2019 ). Most vertebrate genomes encode two related proteins, OTOP2 and OTOP3, that also form proton channels ( Tu et al, 2018 ) and are expressed in a diverse array of tissues, including in the digestive tract, where mutations in the corresponding genes have been linked to disease ( Tu et al, 2018 ; Parikh et al, 2019 ; Qu et al, 2019 ; Yang et al, 2019a ). Functional OTOP channels are conserved across species, including in invertebrates, where they play roles in acid sensing and biomineralization ( Hurle et al, 2011 ; Tu et al, 2018 ; Chang et al, 2021 ; Ganguly et al, 2021 ; Mi et al, 2021 ).…”

Section: Introductionmentioning

confidence: 99%

Structural motifs for subtype-specific pH-sensitive gating of vertebrate otopetrin proton channels

Teng

Kaplan

Liang

et al. 2022

eLife

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Otopetrin (OTOP) channels are proton-selective ion channels conserved among vertebrates and invertebrates, with no structural similarity to other ion channels. There are three vertebrate OTOP channels (OTOP1, OTOP2, and OTOP3), of which one (OTOP1) functions as a sour taste receptor. Whether extracellular protons gate OTOP channels, in addition to permeating them, was not known. Here, we compare the functional properties of the three murine OTOP channels using patch-clamp recording and cytosolic pH microfluorimetry. We find that OTOP1 and OTOP3 are both steeply activated by extracellular protons, with thresholds of pHo <6.0 and 5.5, respectively, and kinetics that are pH-dependent. In contrast, OTOP2 channels are broadly active over a large pH range (pH 5 pH 10) and carry outward currents in response to extracellular alkalinization (>pH 9.0). Strikingly, we could change the pH-sensitive gating of OTOP2 and OTOP3 channels by swapping extracellular linkers that connect transmembrane domains. Swaps of extracellular linkers in the N domain, comprising transmembrane domains 1–6, tended to change the relative conductance at alkaline pH of chimeric channels, while swaps within the C domain, containing transmembrane domains 7–12, tended to change the rates of OTOP3 current activation. We conclude that members of the OTOP channel family are proton-gated (acid-sensitive) proton channels and that the gating apparatus is distributed across multiple extracellular regions within both the N and C domains of the channels. In addition to the taste system, OTOP channels are expressed in the vertebrate vestibular and digestive systems. The distinct gating properties we describe may allow them to subserve varying cell-type specific functions in these and other biological systems.

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“…The expression of CA7 was downregulated in colorectal cancer and correlated with disease progression (Yang et al, 2015 ). Proton-selective channel OTOP2 also acts a tumor suppressor gene in colorectal cancer (Qu et al, 2019 ). CFTR channel is essential for high-volume fluid secretion of water, chloride and bicarbonate in the intestine (Moran, 2017 ).…”

Section: Discussionmentioning

confidence: 99%

Cross-species single-cell transcriptomic analysis reveals divergence of cell composition and functions in mammalian ileum epithelium

Wang

et al. 2022

Cell Regen

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Animal models are widely used for biomedical studies and drug evaluation. The small intestine plays key roles in nutrient absorption, hormone secretion, microbiota defense and drug absorption and metabolism. Although the intestinal structure of mammals is conserved, the differences on epithelial cell composition, functional assignments and drug absorption among mammals are largely unknown. Here, cross-species analysis of single-cell transcriptomic atlas of the ileum epithelium from mouse, rat, pig, macaque and human reveals the conserved and differential cell types and functions among species, identifies a new CA7+ cell type in pig, macaque and human ileum, uncovers the distinct expression pattern in enterocytes, enteroendocrine cells and Paneth cells, and defines the conserved and species-specific intestinal stem cell signature genes. The examination of drug absorption across species suggests that drug metabolism in mouse ileum is closer to human while drug transport in macaque ileum is more similar to human. Together, our data provide the comprehensive information about cell composition and functional assignments in five species, and offer the valuable guidance for animal model selection and drug testing.

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Wild‐type p53 regulates OTOP2 transcription through DNA loop alteration of the promoter in colorectal cancer

Cited by 14 publications

References 18 publications

Right and left-sided colon cancers - specificity of molecular mechanisms in tumorigenesis and progression

Right and left-sided colon cancers - specificity of molecular mechanisms in tumorigenesis and progression

Structural motifs for subtype-specific pH-sensitive gating of vertebrate otopetrin proton channels

Cross-species single-cell transcriptomic analysis reveals divergence of cell composition and functions in mammalian ileum epithelium

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