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A novel mouse model of PMS2 founder mutation that causes mismatch repair defect due to aberrant splicing

  1. Author:
    Biswas,Kajal
    Couillard, Martin
    Cavallone, Luca
    Burkett,Sandra
    Stauffer,Stacey
    Martin, Betty K.
    Southon,Eileen
    Reid,Susan
    Plona,Teri
    Baugher,Ryan
    Mellott,Stephanie
    Pike,Kristen
    Albaugh,Mary
    Maedler-Kron, Chelsea
    Hamel, Nancy
    Tessarollo,Lino
    Marcus, Victoria
    Foulkes, William D.
    Sharan,Shyam

  2. Author Address

    NCI, Mouse Canc Genet Program, Ctr Canc Res, NIH, Frederick, MD 21701 USA.McGill Univ, Lady Davis Inst, Jewish Gen Hosp, Montreal, PQ, Canada.Leidos Biomed Res Inc, Frederick Natl Lab Canc Res, Frederick, MD 21702 USA.Leidos Biomed Res Inc, Frederick Natl Lab Canc Res, CLIA Mol Diagnost Lab, Frederick, MD USA.McGill Univ, Dept Pathol, Montreal, PQ, Canada.McGill Univ, Dept Oncol, Montreal, PQ, Canada.McGill Univ, Dept Human Genet, Montreal, PQ, Canada.McGill Univ, Jewish Gen Hosp, Dept Med Genet, Montreal, PQ H3T 1E2, Canada.McGill Univ, McGill Univ Hlth Ctr, Dept Med Genet, Res Inst, Montreal, PQ H4A 3J1, Canada.McGill Univ, McGill Univ Hlth Ctr, Canc Res Program, Res Inst, Montreal, PQ H4A 3J1, Canada.
    1. Year: 2021
    2. Date: Sep 6
  2. Journal: Cell Death & Disease
  3. SPRINGERNATURE,
    1. 12
    2. 9
  5. Type of Article: Article
  6. Article Number: 838
  7. ISSN: 2041-4889
  1. Abstract:

    Hereditary non-polyposis colorectal cancer, now known as Lynch syndrome (LS) is one of the most common cancer predisposition syndromes and is caused by germline pathogenic variants (GPVs) in DNA mismatch repair (MMR) genes. A common founder GPV in PMS2 in the Canadian Inuit population, NM_000535.5: c.2002A>G, leads to a benign missense (p.I668V) but also acts as a de novo splice site that creates a 5 bp deletion resulting in a truncated protein (p.I668*). Individuals homozygous for this GPV are predisposed to atypical constitutional MMR deficiency with a delayed onset of first primary malignancy. We have generated mice with an equivalent germline mutation (Pms2c.1993A>G) and demonstrate that it results in a splicing defect similar to those observed in humans. Homozygous mutant mice are viable like the Pms2 null mice. However, unlike the Pms2 null mice, these mutant mice are fertile, like humans homozygous for this variant. Furthermore, these mice exhibit a significant increase in microsatellite instability and intestinal adenomas on an Apc mutant background. Rectification of the splicing defect in human and murine fibroblasts using antisense morpholinos suggests that this novel mouse model can be valuable in evaluating the efficacy aimed at targeting the splicing defect in PMS2 that is highly prevalent among the Canadian Inuits.

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External Sources

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  2. DOI: 10.1038/s41419-021-04130-8
  3. PMID: 34489406
  4. PMCID: PMC8421400
  5. View record in Web of ScienceĀ®
  6. WOS: 000694247400002

Library Notes

  1. Fiscal Year: FY2021-2022
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