García-Solorio Joaquín, Martínez-Villegas Octavio, Rodríguez-Corona Ulises, Molina-Garay Carolina, Jiménez-Olivares Marco, Carrillo-Sanchez Karol, Mendoza-Caamal Elvia C, Muñoz-Rivas Anallely, Villegas-Torres Beatriz E, Cervera Alejandra, Flores-Lagunes Luis L, Alaez-Verson Carmen
Laboratorio de Diagnóstico Genómico, Instituto Nacional de Medicina Genómica (INMEGEN), Mexico City, Mexico.
Departamento de hemato-oncología pediátrica, Unidad Médicade Alta Especialidad Hospital de Ginecología Pediatría No 48, Centro Médico del Bajío, León, Guanajuato, Mexico.
Front Oncol. 2024 Mar 20;14:1355335. doi: 10.3389/fonc.2024.1355335. eCollection 2024.
B-cell acute lymphoblastic leukemia (B-ALL) is one of the most common childhood cancers worldwide. Although most cases are sporadic, some familial forms, inherited as autosomal dominant traits with incomplete penetrance, have been described over the last few years. Germline pathogenic variants in transcription factors such as , and have been identified as causal in familial forms. The proband was a 7-year-old Mexican girl diagnosed with high-risk B-ALL at five years and 11 months of age. Family history showed that the proband's mother had high-risk B-ALL at 16 months of age. She received chemotherapy and was discharged at nine years of age without any evidence of recurrence of leukemia. The proband's father was outside the family nucleus, but no history of leukemia or cancer was present up to the last contact with the mother. We performed exome sequencing on the proband and the proband's mother and identified the variant NM_016734.3:c.963del: p.(Ala322LeufsTer11), located in the transactivation domain of the PAX5 protein. The variant was classified as probably pathogenic according to the ACMG criteria. To the best of our knowledge, this is the first Mexican family with an inherited increased risk of childhood B-ALL caused by a novel germline pathogenic variant of . Identifying individuals with a hereditary predisposition to cancer is essential for modern oncological practice. Individuals at high risk of leukemia would benefit from hematopoietic stem cell transplantation, but family members carrying the pathogenic variant should be excluded as hematopoietic stem cell donors.
B细胞急性淋巴细胞白血病(B-ALL)是全球最常见的儿童癌症之一。尽管大多数病例是散发性的,但在过去几年中,已经描述了一些家族性形式,其作为常染色体显性性状遗传,具有不完全外显率。转录因子如 、 和 的种系致病变异已被确定为家族性形式的病因。先证者是一名7岁的墨西哥女孩,在5岁11个月时被诊断为高危B-ALL。家族史显示,先证者的母亲在16个月大时患有高危B-ALL。她接受了化疗,9岁时出院,没有白血病复发的任何迹象。先证者的父亲不在家庭核心成员范围内,但在与母亲的最后一次联系时,没有白血病或癌症病史。我们对先证者和先证者的母亲进行了外显子组测序,确定了位于PAX5蛋白反式激活结构域的变异NM_016734.(此处原文有误,推测应为NM_016734.3):c.963del:p.(Ala322LeufsTer11)。根据ACMG标准,该变异被分类为可能致病。据我们所知,这是第一个因 的新型种系致病变异而导致儿童B-ALL遗传风险增加的墨西哥家族。识别具有癌症遗传易感性的个体对于现代肿瘤学实践至关重要。白血病高危个体将从造血干细胞移植中受益,但携带致病变异的家庭成员应被排除作为造血干细胞供体。
