Gα12 and Gα13: Versatility in Physiology and Pathology

Guo, Pengfei; Tai, Yu Tzu; Wang, Manman; Sun, Hairui; Zhang, Lingling; Wei, Wei; Xiang, Yang; Wang, Qingtong

doi:10.3389/fcell.2022.809425

Cited by 9 publications

(3 citation statements)

References 205 publications

(274 reference statements)

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“…This leads to the activation of a host of downstream transcription factors, notably NF-κB, a major player in the expression of genes encoding inflammatory factors ( 33 ). In the case of Gα12/13, activation leads to Rho-mediated cytoskeleton reorganization, collaborating with Gβγ to regulate immune cell chemotaxis to inflammation sites - these actions primarily result in pro-inflammatory effects ( 34 , 35 ). Gαq coupled with GPR35 directly inhibits the PI3K catalytic subunit and then suppresses Akt activation.…”

Section: Gpr35 Involved Inflammation-related Pathwaysmentioning

confidence: 99%

GPR35 acts a dual role and therapeutic target in inflammation

Wu,

Zhang,

Fan

et al. 2023

Front. Immunol.

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GPR35 is a G protein-coupled receptor with notable involvement in modulating inflammatory responses. Although the precise role of GPR35 in inflammation is not yet fully understood, studies have suggested that it may have both pro- and anti-inflammatory effects depending on the specific cellular environment. Some studies have shown that GPR35 activation can stimulate the production of pro-inflammatory cytokines and facilitate the movement of immune cells towards inflammatory tissues or infected areas. Conversely, other investigations have suggested that GPR35 may possess anti-inflammatory properties in the gastrointestinal tract, liver and certain other tissues by curbing the generation of inflammatory mediators and endorsing the differentiation of regulatory T cells. The intricate role of GPR35 in inflammation underscores the requirement for more in-depth research to thoroughly comprehend its functional mechanisms and its potential significance as a therapeutic target for inflammatory diseases. The purpose of this review is to concurrently investigate the pro-inflammatory and anti-inflammatory roles of GPR35, thus illuminating both facets of this complex issue.

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Section: Gpr35 Involved Inflammation-related Pathwaysmentioning

confidence: 99%

GPR35 acts a dual role and therapeutic target in inflammation

Wu,

Zhang,

Fan

et al. 2023

Front. Immunol.

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“…P2RY10 has been demonstrated to activate GNA12/13 signaling, which is crucial for the proliferation of tumor cells [18,17]. To further investigate the downstream pathways of P2RY10, LoVo cells overexpressing GNA13 were generated.…”

Section: The Role Of Gna13 In the Expression Of P2ry10 And Gna13 In L...mentioning

confidence: 99%

“…In addition, high P2RY10 expression can upregulate the expression of GNA12 and GNA13, which are essential for tumor cell proliferation [17]. It has been reported that GNA12/13 activation can accelerate proliferation and tumor formation in small-cell lung carcinoma, ovarian cancer, and hepatocellular carcinoma cells [18]. Therefore, the current study first determined the levels of P2RY10 and lncRNA TRG-AS1 in normal and CRC cell lines, and then explored the functions of TRG-AS1 and P2RY10 in CRC development in vitro and in vivo.…”

Section: Introductionmentioning

confidence: 99%

The lncRNA TRG-AS1 promotes the growth of colorectal cancer cells through the regulation of P2RY10/GNA13

Luo¹,

Zhuang²,

Sun³

et al. 2023

Preprint

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Purpose: The lncRNA TRG-AS1 and its co-expressed gene P2RY10 are important for colorectal cancer (CRC) occurrence and development. The purpose of our research was to explore the roles of TRG-AS1 and P2RY10 in CRC progression. Methods: The abundance of TRG-AS1 and P2RY10 was determined in CRC cell lines. LoVo cells were transfected with si-TRG-AS1 and si-P2RY10 constructs. Subsequently, the viability, colony formation, and migration of the transfected cells were analyzed using cell counting kit-8, clonogenicity, and scratch-wound/Transwell assays, respectively. Cells overexpressing GNA13 were used to further explore the relationship between TRG-AS1 and P2RY10 along with their downstream functions. Finally, nude mice were injected with different transfected cell types to observe tumor formation in vivo. Results: TRG-AS1 and P2RY10 were significantly upregulated in HT-29 and LoVo compared to FHC cells. TRG-AS1 knockdown and P2RY10 silencing suppressed the viability, colony formation, and migration of LoVo cells. TRG-AS1 knockdown downregulated the expression of P2RY10, GNA12, and GNA13, while P2RY10 silencing downregulated the expression of TRG-AS1, GNA12, and GNA13. Additionally, GNA13 overexpression reversed the cell growth and gene expression changes in LoVo cells induced by TRG-AS1 knockdown or P2RY10 silencing. In vivo experiments revealed that CRC tumor growth was suppressed by TRG-AS1 knockdown and P2RY10 silencing. Conclusions: TRG-AS1 knockdown repressed the growth of CRC cells by regulating P2RY10 and GNA13 expression, thereby controlling CRC occurrence and development.

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Divergent Approaches Toward Drug Discovery and Development

Koul

2023

The Quintessence of Basic and Clinical Research and Scientific Publishing

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Gα12 and Gα13: Versatility in Physiology and Pathology

Cited by 9 publications

References 205 publications

GPR35 acts a dual role and therapeutic target in inflammation

GPR35 acts a dual role and therapeutic target in inflammation

The lncRNA TRG-AS1 promotes the growth of colorectal cancer cells through the regulation of P2RY10/GNA13

Divergent Approaches Toward Drug Discovery and Development

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