TP53 PATHOGENIC VARIANTS RELATED TO CANCER-Reference-Cited by-同舟云学术

TP53 PATHOGENIC VARIANTS RELATED TO CANCER

Published:2019-12-28 Issue:2 Volume:30 Page:27-40
ISSN:1852-6233
Container-title:Journal of Basic and Applied Genetics
language:
Short-container-title:BAG

Author:

Rosero C.Y.¹,Mejia L.G.²,Corredor M.³

Affiliation:

1. Interdisciplinary Research Group in Health and Disease, Medicine Faculty, Universidad Cooperativa de Colombia, San Juan de Pasto, Nariño, Colombia

2. Interdisciplinary Research Group in Health and Disease, Medicine Faculty, Universidad Cooperativa de Colombia, San Juan de Pasto, Nariño, Colombia.

3. Genetics and Biochemistry of Microorganisms, Natural and Exact Sciences Faculty, Biology Institute, Universidad de Antioquia, Medellín, Colombia. Genetics, Regeneration and Cancer, GRC, Natural and Exact Sciences Faculty, Biology Institute, Universidad de Antioquia, Medellín, Colombia.

Abstract

TP53 or P53 is a tumor suppressor gene known as the “genome guardian”, responsible for inducing cell response to DNA damage, by stopping the cell cycle in case of mutation, activating DNA repair enzymes, initiating senescence and activation of apoptosis. Mutations in the gene sequence can cause non-synonymous mutations or errors in the reading frame by insertion, deletion or displacement of nucleotides: e.g., c.358A>G mutation in exon 4 and variants located in exons 9 and 10 of the TD domain. Therefore, in this review, we will see that changes in the reading frame, including the loss of one or two base pairs could prevent accurate transcription or changes in the structure and function of the protein, and could completely impair reparation function. These changes promote self-sufficiency in growth signaling, insensitivity to anti-growth signals, and evasion of apoptosis, resulting in limitless replication and induction of metastatic angiogenesis, generating as a consequence the proliferation of tumor, neoplastic, and lymphoid cells. Taking into account the importance of TP53 in the regulation of the cell cycle, the objective of this review is to update information related to the role of this gene in the development of cancer and the description of genetic variations. Key words: Neoplasms, nuclear phosphoprotein p53, Tumor Suppressor, mutation, Clinvar, Uniprot

Publisher

Sociedad Argentina de Genetica

Subject

Genetics (clinical),Genetics,Applied Microbiology and Biotechnology,Biotechnology

Reference86 articles.

1. Adrain C., Creagh E. (2001) Apoptosis-associated release of Smac/DIABLO from mitochondria requires active caspases and is blocked by Bcl-2. EMBO J. 20 (23): 6627-6636.

2. Alpízar W., Sierra R., Cuenca P., Une C., Mena F., Pérez G. (2005) Asociación del polimorfismo del codón 72 del gen p53 con el riesgo de cáncer gástrico en una población de alto riesgo de Costa Rica. Rev. Biol. Trop. 53 (3-4): 317-324.

3. Audrezet M.P., Robaszkiewicz M., Mercier B., Nousbaum J.B., Hardy E., Bail J.P. (1996) Molecular analysis of the TP53 gene in Barrett’s adenocarcinoma. Hum. Mutat. 7: 109-113.

4. Azuma K., Shichijo S., Itoh K. (2002) Identification of a tumor-rejection antigen recognized by HLA-B46 restricted CTL. Submitted (MAR2002) to the EMBL/GenBank/DDBJ databases.

5. Bai L. and Zhu W. (2006) p53: Structure, Function and therapeutic applications. J. Cancer Mol. 2 (4): 141-153.