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C77G in PTPRC (CD45) is no risk allele for ovarian cancer, but associated with less aggressive disease
Author(s) -
Johannes Landskron,
Sigrid Marie Kraggerud,
Elisabeth Wik,
Anne Dørum,
Merete Bjørnslett,
Espen Melum,
Øystein Helland,
Line Bjørge,
Ragnhild A. Lothe,
Helga B. Salvesen,
Kjetil Taskén
Publication year - 2017
Publication title -
plos one
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.99
H-Index - 332
ISSN - 1932-6203
DOI - 10.1371/journal.pone.0182030
Subject(s) - ovarian cancer , exon , cancer , alternative splicing , allele , biology , oncology , population , cohort , allele frequency , medicine , cancer research , genetics , gene , environmental health
The pan lymphocyte marker CD45 exists in various isoforms arising from alternative splicing of the exons 4, 5 and 6. While naïve T cells express CD45RA translated from an mRNA containing exon 4, exons 4–6 are spliced out to encode the shorter CD45R0 in antigen-experienced effector/memory T cells. The SNP C77G (rs17612648) is located in exon 4 and blocks the exon’s differential splicing from the pre-mRNA, enforcing expression of CD45RA. Several studies have linked C77G to autoimmune diseases but lack of validation in other cohorts has left its role elusive. An incidental finding in an ovarian cancer patient cohort from West Norway (Bergen region, n = 312), suggested that the frequency of C77G was higher among ovarian cancer patients than in healthy Norwegians (n = 1,357) (3.0% vs. 1.8% allele frequency). However, this finding could not be validated in a larger patient cohort from South-East Norway (Oslo region, n = 1,198) with 1.2% allele frequency. Hence, C77G is not associated with ovarian cancer in the Norwegian population. However, its frequency was increased in patients with FIGO stage II, endometrioid histology or an age at diagnosis of 60 years or older indicating a possible association with a less aggressive cancer type.

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