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The oncogenic potential of Rab-like protein 1A (RBEL1A) GTPase: The first review of RBEL1A research with future research directions and challenges

Research on Rab-like protein 1A (RBEL1A) in the past two decades highlighted the oncogenic properties of this gene. Despite the emerging evidence, its importance in cancer biology was underrated. This is the first RBEL1A critical review covering its discovery, biochemistry, physiological functions,...

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Autores principales: Lui, Ki, Huang, Ying, Sheikh, M. Saeed, Cheung, Kwok-Kuen, Tam, Wing Yip, Sun, Keng-Ting, Cheng, Ka Ming, Ng, Winnie Wing Man, Loh, Anthony Wai-Keung
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10622986/
https://www.ncbi.nlm.nih.gov/pubmed/37928422
http://dx.doi.org/10.7150/jca.84267
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author Lui, Ki
Huang, Ying
Sheikh, M. Saeed
Cheung, Kwok-Kuen
Tam, Wing Yip
Sun, Keng-Ting
Cheng, Ka Ming
Ng, Winnie Wing Man
Loh, Anthony Wai-Keung
author_facet Lui, Ki
Huang, Ying
Sheikh, M. Saeed
Cheung, Kwok-Kuen
Tam, Wing Yip
Sun, Keng-Ting
Cheng, Ka Ming
Ng, Winnie Wing Man
Loh, Anthony Wai-Keung
author_sort Lui, Ki
collection PubMed
description Research on Rab-like protein 1A (RBEL1A) in the past two decades highlighted the oncogenic properties of this gene. Despite the emerging evidence, its importance in cancer biology was underrated. This is the first RBEL1A critical review covering its discovery, biochemistry, physiological functions, and clinical insights. RBEL1A expression at the appropriate levels appears essential in normal cells and tissues to maintain chromosomal stability; however, its overexpression is linked to tumorigenesis. Furthermore, the upstream and downstream targets of the RBEL1A signaling pathways will be discussed. Mechanistically, RBEL1A promotes cell proliferation signals by enhancing the Erk1/2, Akt, c-Myc, and CDK pathways while blunting the apoptotic signals via inhibitions on p53, Rb, and caspase pathways. More importantly, this review covers the clinical relevance of RBEL1A in the cancer field, such as drug resistance and poor overall survival rate. Also, this review points out the bottle-necks of the RBEL1A research and its future research directions. It is becoming clear that RBEL1A could potentially serve as a valuable target of anticancer therapy. Genetic and pharmacological researches are expected to facilitate the identification and development of RBEL1A inhibitors as cancer therapeutics in the future, which could undoubtedly improve the management of human malignancy.
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spelling pubmed-106229862023-11-04 The oncogenic potential of Rab-like protein 1A (RBEL1A) GTPase: The first review of RBEL1A research with future research directions and challenges Lui, Ki Huang, Ying Sheikh, M. Saeed Cheung, Kwok-Kuen Tam, Wing Yip Sun, Keng-Ting Cheng, Ka Ming Ng, Winnie Wing Man Loh, Anthony Wai-Keung J Cancer Review Research on Rab-like protein 1A (RBEL1A) in the past two decades highlighted the oncogenic properties of this gene. Despite the emerging evidence, its importance in cancer biology was underrated. This is the first RBEL1A critical review covering its discovery, biochemistry, physiological functions, and clinical insights. RBEL1A expression at the appropriate levels appears essential in normal cells and tissues to maintain chromosomal stability; however, its overexpression is linked to tumorigenesis. Furthermore, the upstream and downstream targets of the RBEL1A signaling pathways will be discussed. Mechanistically, RBEL1A promotes cell proliferation signals by enhancing the Erk1/2, Akt, c-Myc, and CDK pathways while blunting the apoptotic signals via inhibitions on p53, Rb, and caspase pathways. More importantly, this review covers the clinical relevance of RBEL1A in the cancer field, such as drug resistance and poor overall survival rate. Also, this review points out the bottle-necks of the RBEL1A research and its future research directions. It is becoming clear that RBEL1A could potentially serve as a valuable target of anticancer therapy. Genetic and pharmacological researches are expected to facilitate the identification and development of RBEL1A inhibitors as cancer therapeutics in the future, which could undoubtedly improve the management of human malignancy. Ivyspring International Publisher 2023-10-02 /pmc/articles/PMC10622986/ /pubmed/37928422 http://dx.doi.org/10.7150/jca.84267 Text en © The author(s) https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/). See http://ivyspring.com/terms for full terms and conditions.
spellingShingle Review
Lui, Ki
Huang, Ying
Sheikh, M. Saeed
Cheung, Kwok-Kuen
Tam, Wing Yip
Sun, Keng-Ting
Cheng, Ka Ming
Ng, Winnie Wing Man
Loh, Anthony Wai-Keung
The oncogenic potential of Rab-like protein 1A (RBEL1A) GTPase: The first review of RBEL1A research with future research directions and challenges
title The oncogenic potential of Rab-like protein 1A (RBEL1A) GTPase: The first review of RBEL1A research with future research directions and challenges
title_full The oncogenic potential of Rab-like protein 1A (RBEL1A) GTPase: The first review of RBEL1A research with future research directions and challenges
title_fullStr The oncogenic potential of Rab-like protein 1A (RBEL1A) GTPase: The first review of RBEL1A research with future research directions and challenges
title_full_unstemmed The oncogenic potential of Rab-like protein 1A (RBEL1A) GTPase: The first review of RBEL1A research with future research directions and challenges
title_short The oncogenic potential of Rab-like protein 1A (RBEL1A) GTPase: The first review of RBEL1A research with future research directions and challenges
title_sort oncogenic potential of rab-like protein 1a (rbel1a) gtpase: the first review of rbel1a research with future research directions and challenges
topic Review
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10622986/
https://www.ncbi.nlm.nih.gov/pubmed/37928422
http://dx.doi.org/10.7150/jca.84267
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