Marginal Contribution of Pathogenic RAD51D Germline Variants to Pakistani Early-Onset and Familial Breast/Ovarian Cancer Patients.

Journal of cancer & allied specialties Pub Date : 2024-08-16 eCollection Date: 2024-01-01 DOI:10.37029/jcas.v10i2.617
Noor Muhammad, Muhammad Sohail Afzal, Ute Hamann, Muhammad Usman Rashid
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Abstract

Introduction: RAD51D has been reported as a breast cancer (BC) and ovarian cancer (OC) predisposition gene, particularly among Caucasian populations. We studied the prevalence of RAD51D variants in Pakistani BC/OC patients.

Materials and methods: In total, 371 young or familial BC/OC patients were thoroughly analyzed for RAD51D sequence variants using denaturing high-performance liquid chromatography pursued by DNA sequencing of differentially eluted amplicons. We also assessed the pathogenic effects of novel variants using in-silico algorithms. All detected RAD51D variants were investigated in 400 unaffected controls.

Results: No pathogenic RAD51D variant was detected. However, we identified nine unique heterozygous variants. Of these, two missense variants (p.Pro10Leu and p.Ile311Asn) and one intronic variant (c.481-26_23delGTTC) were classified as in silico-predicted variants of uncertain significance, with a frequency of 0.8% (3/371). The p.Pro10Leu variant was detected in a 28-year-old female BC patient of Punjabi ethnic background, whose mother and maternal cousin had BCs at ages 53 and 40, respectively. This variant was also detected in 1/400 (0.25%) healthy controls, where the control subject's daughter had acute lymphoblastic leukemia. The p.Ile311Asn variant was identified in a female BC patient at age 29 of Punjabi ethnicity and in 1/400 (0.25%) healthy controls, where the control subject's daughter had Hodgkin's disease at age 14. A novel intronic variant, c.481-26_-23delGTTC, was found in a 30-year-old Punjabi female BC patient but not in 400 healthy controls.

Conclusion: No pathogenic RAD51D variant was identified in the current study. Our study data suggested a negligible association of RAD51D variants with BC/OC risk in Pakistani women.

致病性 RAD51D 基因变异对巴基斯坦早发和家族性乳腺癌/卵巢癌患者的影响微乎其微。
引言据报道,RAD51D是乳腺癌(BC)和卵巢癌(OC)的易感基因,尤其是在白种人中。我们研究了巴基斯坦 BC/OC 患者中 RAD51D 变异的发生率:采用变性高效液相色谱法对 371 名年轻或家族性 BC/OC 患者的 RAD51D 序列变异进行了全面分析,并对不同洗脱扩增子进行了 DNA 测序。我们还使用体内算法评估了新型变体的致病作用。所有检测到的 RAD51D 变异都在 400 个未受影响的对照组中进行了调查:结果:未检测到致病性 RAD51D 变异。然而,我们发现了 9 个独特的杂合变异。其中,两个错义变异(p.Pro10Leu 和 p.Ile311Asn)和一个内含子变异(c.481-26_23delGTTC)被归类为意义不确定的硅预测变异,频率为 0.8%(3/371)。p.Pro10Leu变异在一名28岁的旁遮普族女性BC患者中检测到,她的母亲和表姐分别在53岁和40岁时患上BC。在 1/400(0.25%)名健康对照者中也检测到了该变异,其中对照者的女儿患有急性淋巴细胞白血病。在一名 29 岁的旁遮普族女性 BC 患者和 1/400 名(0.25%)健康对照者中发现了 p.Ile311Asn 变体,其中对照者的女儿在 14 岁时患有霍奇金病。在一名 30 岁的旁遮普族女性 BC 患者中发现了一个新的内含子变异 c.481-26_-23delGTTC,但在 400 名健康对照中没有发现:本研究未发现致病的 RAD51D 变异。我们的研究数据表明,在巴基斯坦女性中,RAD51D变异与BC/OC风险的关系微乎其微。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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