Literature DB >> 19904757

Parent of origin effects on age at colorectal cancer diagnosis.

Noralane M Lindor1, Kari G Rabe, Gloria M Petersen, Helen Chen, Bharati Bapat, John Hopper, Joanne Young, Mark Jenkins, John Potter, Polly Newcomb, Allyson Templeton, Loic Lemarchand, John Grove, Michael R Burgio, Robert Haile, Jane Green, Michael O Woods, Daniela Seminara, Paul J Limburg, Stephen N Thibodeau.   

Abstract

Genomic imprinting refers to a parent-of-origin specific effect on gene expression. At least 1% of genes in the human genome are modulated in this manner. We sought evidence for genomic imprinting in colorectal cancer by studying the ages at diagnosis in the offspring of 2,061 parent-child pairs in which both parent and child were affected by nonsyndromic colorectal cancer. Families were ascertained through the colon Cancer Family Registry [http://epi.grants.cancer.gov/CFR/] from both population-based and clinic-based sources. We found that the affected offspring of affected fathers were on average younger than offspring of affected mothers (55.8 vs. 53.7 years; p = 0.0003), but when divided into sons and daughters, this difference was driven entirely by younger age at diagnosis in daughters of affected fathers compared to sons (52.3 years vs. 55.1 years; p = 0.0004). A younger age at diagnosis in affected daughters of affected fathers was also observable in various subsets including families that met Amsterdam II Criteria, families that did not meet Amsterdam Criteria, and in families with documented normal DNA mismatch repair in tumors. Imprinting effects are not expected to be affected by the sex of the offspring. Possible explanations for these unexpected findings include: (i) an imprinted gene on the pseudoautosomal regions of the X chromosome; (ii) an imprinted autosomal gene that affects a sex-specific pathway; or (iii) an X-linked gene unmasked because of colonic tissue-specific preferential inactivation of the maternal X chromosome.

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Year:  2010        PMID: 19904757      PMCID: PMC2877160          DOI: 10.1002/ijc.25037

Source DB:  PubMed          Journal:  Int J Cancer        ISSN: 0020-7136            Impact factor:   7.396


  19 in total

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4.  Effect of Turner's syndrome and X-linked imprinting on cognitive status: analysis based on pedigree data.

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Review 5.  Imprinted noncoding RNAs.

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7.  Lower cancer incidence in Amsterdam-I criteria families without mismatch repair deficiency: familial colorectal cancer type X.

Authors:  Noralane M Lindor; Kari Rabe; Gloria M Petersen; Robert Haile; Graham Casey; John Baron; Steve Gallinger; Bharati Bapat; Melyssa Aronson; John Hopper; Jeremy Jass; Loic LeMarchand; John Grove; John Potter; Polly Newcomb; Jonathan P Terdiman; Peggy Conrad; Gabriella Moslein; Richard Goldberg; Argyrios Ziogas; Hoda Anton-Culver; Mariza de Andrade; Kim Siegmund; Stephen N Thibodeau; Lisa A Boardman; Daniela Seminara
Journal:  JAMA       Date:  2005-04-27       Impact factor: 56.272

8.  Loss of IGF2 imprinting: a potential marker of colorectal cancer risk.

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Review 9.  Uniparental disomy, isodisomy, and imprinting: probable effects in man and strategies for their detection.

Authors:  E Engel; C D DeLozier-Blanchet
Journal:  Am J Med Genet       Date:  1991-09-15

Review 10.  Imprinted genes: identification by chromosome rearrangements and post-genomic strategies.

Authors:  Rebecca J Oakey; Colin V Beechey
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  6 in total

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3.  Dependence of colorectal cancer risk on the parent-of-origin of mutations in DNA mismatch repair genes.

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4.  Individual having a parent with early-onset gastric cancer may need screening at younger age.

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Review 5.  Molecular alterations in gastric cancer with special reference to the early-onset subtype.

Authors:  Małgorzata Skierucha; Anya Na Milne; G Johan A Offerhaus; Wojciech P Polkowski; Ryszard Maciejewski; Robert Sitarz
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6.  Do the risks of Lynch syndrome-related cancers depend on the parent of origin of the mutation?

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  6 in total

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