AI Article Synopsis

  • Multiple polyposes are complex diseases characterized by the development of cancerous intestinal polyps, with a focus on identifying genetic mutations affecting risk, particularly in Polish patients.
  • Researchers studied the p.Q82* mutation in 644 polyposis patients and 634 controls, finding the variant present in some patients, indicating a potential association with increased colorectal cancer risk.
  • The study highlights the need for further genetic screening, especially for patients with the homozygous p.Q82* variant, as it appeared more frequently in patients without other identified mutations, suggesting it could be an important marker.

Article Abstract

Multiple polyposes are heterogeneous diseases with different underlying molecular backgrounds, sharing a common symptom: the presence of transforming into cancerous intestinal polyps. Recent reports have indicated biallelic mutations in the gene, which is involved in base excision repair (BER), as predisposing to an elevated risk of colorectal cancer (CRC). We aimed to evaluate the significance of the p.Q82* truncating variant in predisposition to intestinal polyposis by assessing its frequency in polyposis patients. We genotyped 644 Polish patients and 634 control DNA samples using high-resolution melting analysis (HRM) and Sanger sequencing. We found the p.Q82* variant in four polyposis patients; in three, it was homozygous (OR = 6.90, value = 0.202). Moreover, the p.R92C mutation was detected in one patient. We also looked more closely at the disease course in patients carrying mutations. Two homozygous patients also presented other neoplasia. In the family case, we noticed the earlier presence of polyps in the proband and early hepatoblastoma in his brother. We cannot univocally confirm the relationship of p.Q82* with an increased risk of CRC. However, homozygous p.Q82* was more frequent by 10-fold in patients without other mutations identified, which makes gene screening in this group reasonable.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10572874PMC
http://dx.doi.org/10.3390/ijms241914548DOI Listing

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