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Identification of DeltaN isoform and polyadenylation site choice variants in molluscan p63/p73-like homologues.

作者信息

Muttray Annette F, Cox Rachel L, Reinisch Carol L, Baldwin Susan A

机构信息

Laboratory of Aquatic Biomedicine, Marine Biological Laboratory, Woods Hole, Massachusetts 02543, USA.

出版信息

Mar Biotechnol (NY). 2007 Mar-Apr;9(2):217-30. doi: 10.1007/s10126-006-6045-1. Epub 2007 Jan 22.


DOI:10.1007/s10126-006-6045-1
PMID:17242983
Abstract

The p53 family of transcription factors has been implicated in many vertebrate cancers. Altered p53 and p73 protein expression observed in leukemic cells of molluscs suggests that these transcription factors might be involved in invertebrate cancers as well. Here, we fully characterize the mRNA of four novel p53-like variants in the bivalve molluscs Mytilus trossulus (bay mussel) and Mytilus edulis (blue mussel). These species, widely used for environmental assessment, develop a hemic neoplasia (leukemia) that is frequently fatal. The correlation between expression of p53 and its close relative p73 and onset of molluscan leukemia was documented previously. We report the sequences of two distinct and novel p63/p73-like mRNAs, amplified by polymerase chain reaction (PCR) from both species. One of the p63/p73-like isoforms contains a 360 nt truncation in the 5' coding region. Based on this truncation and concomitant lack of a transactivation (TA) domain, we designate this variant as a DeltaNp63/p73-like isoform: the first to be reported in an invertebrate species. In mammalian species, DeltaNp73 potently inhibits the tumor-suppressive function of p73 and p53, and its overexpression serves as a robust marker for mammalian cancer. In addition, we report on the occurrence of alternate polyadenylation sites in the molluscan p63/p73: one proximal and one distal site, which differ by 1260 nt. We hypothesize that differential expression of various molluscan p63/p73-like isoforms, controlled in part by polyadenylation site choice variation, may help to interpret the apparently opposing roles of this gene in the development of cancer. Overall, this research further illustrates the utility of the molluscan model for studies involving the molecular mechanisms of oncogenesis in naturally occurring populations. The data presented here require a revisiting of hypotheses regarding evolution of the p53 gene family. Current hypotheses indicate that (1) the protostome gene family does not contain an intronic promoter for DeltaN expression and (2) p53 gene duplication did not occur in protostomes. Our characterization of DeltaN p63/73 in mussel suggests that molluscan p53 gene family members have acquired an intronic promoter or splicing mechanism, either by invention that predates the evolutionary split of deuterostomes from protostomes, or by parallel evolution. Our data also show that Mytilus p53, p63/p73, and DeltaNp63/p73 are identical in their core regions with variation limited to their C- and N-terminals, supporting the notion that alternative splicing, intronic promoter usage, and polyadenylation site choice may lead to expression of distinct isoforms originating from one common gene.

摘要

相似文献

[1]
Identification of DeltaN isoform and polyadenylation site choice variants in molluscan p63/p73-like homologues.

Mar Biotechnol (NY). 2007

[2]
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[3]
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[4]
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[5]
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[6]
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[7]
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[8]
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[9]
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[10]
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引用本文的文献

[1]
Transcriptomics of mussel transmissible cancer MtrBTN2 suggests accumulation of multiple cancer traits and oncogenic pathways shared among bilaterians.

Open Biol. 2023-10

[2]
Identification of relevant cancer related-genes in the flat oyster Ostrea edulis affected by disseminated neoplasia.

Mar Biotechnol (NY). 2012-7-26

[3]
Recognition and suppression of transfected plasmids by protein ZNF511-PRAP1, a potential molecular barrier to transgene expression.

Mol Ther. 2011-5-3

[4]
Phylogeny and function of the invertebrate p53 superfamily.

Cold Spring Harb Perspect Biol. 2010-5-5

[5]
An invertebrate mdm homolog interacts with p53 and is differentially expressed together with p53 and ras in neoplastic Mytilus trossulus haemocytes.

Comp Biochem Physiol B Biochem Mol Biol. 2010-4-22

[6]
Proteomics identification of azaspiracid toxin biomarkers in blue mussels, Mytilus edulis.

Mol Cell Proteomics. 2009-4-23

本文引用的文献

[1]
p53 isoforms can regulate p53 transcriptional activity.

Genes Dev. 2005-9-15

[2]
The promyelocytic leukaemia protein tumour suppressor functions as a transcriptional regulator of p63.

Oncogene. 2005-10-20

[3]
Identification and phylogenetic comparison of p53 in two distinct mussel species (Mytilus).

Comp Biochem Physiol C Toxicol Pharmacol. 2005-2

[4]
A large-scale analysis of mRNA polyadenylation of human and mouse genes.

Nucleic Acids Res. 2005-1-12

[5]
Expression of deltaNp73 predicts poor prognosis in lung cancer.

Clin Cancer Res. 2004-10-15

[6]
Abnormalities of p51, p53, FLT3 and N-ras genes and their prognostic value in relapsed acute myeloid leukemia.

J Nippon Med Sch. 2004-8

[7]
p63 and p73: roles in development and tumor formation.

Mol Cancer Res. 2004-7

[8]
Transdominant DeltaTAp73 isoforms are frequently up-regulated in ovarian cancer. Evidence for their role as epigenetic p53 inhibitors in vivo.

Cancer Res. 2004-4-1

[9]
p73, the "assistant" guardian of the genome?

Ann N Y Acad Sci. 2003-12

[10]
Metazoan evolution: some animals are more equal than others.

Curr Biol. 2004-2-3

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