bims-lifras Biomed News
on Li-Fraumeni syndrome
Issue of 2022–05–08
four papers selected by
Joanna Zawacka-Pankau, Karolinska Institutet
  1. Unraveling the Genetic Architecture of Hepatoblastoma Risk: Birth Defects and Increased Burden of Germline Damaging Variants in Gastrointestinal/Renal Cancer Predisposition and DNA Repair Genes.
  2. Germline predisposition to pediatric Ewing sarcoma is characterized by inherited pathogenic variants in DNA damage repair genes.
  3. Germline Mutational Landscape in Chinese Patients With Advanced Breast Cancer.
  4. Convergence between germline and somatic mutations in pancreatic neuroendocrine tumors.
  1. Front Genet. 2022 ;13 858396
    Unraveling the Genetic Architecture of Hepatoblastoma Risk: Birth Defects and Increased Burden of Germline Damaging Variants in Gastrointestinal/Renal Cancer Predisposition and DNA Repair Genes.
    Talita Aguiar, Anne Teixeira, Marília O Scliar, Juliana Sobral de Barros, Renan B Lemes, Silvia Souza, Giovanna Tolezano, Fernanda Santos, Israel Tojal, Monica Cypriano, Silvia Regina Caminada de Toledo, Eugênia Valadares, Raquel Borges Pinto, Osvaldo Afonso Pinto Artigalas, Joaquim Caetano de Aguirre Neto, Estela Novak, Lilian Maria Cristofani, Sofia M Miura Sugayama, Vicente Odone, Isabela Werneck Cunha, Cecilia Maria Lima da Costa, Carla Rosenberg, Ana Krepischi.
      The ultrarare hepatoblastoma (HB) is the most common pediatric liver cancer. HB risk is related to a few rare syndromes, and the molecular bases remain elusive for most cases. We investigated the burden of rare damaging germline variants in 30 Brazilian patients with HB and the presence of additional clinical signs. A high frequency of prematurity (20%) and birth defects (37%), especially craniofacial (17%, including craniosynostosis) and kidney (7%) anomalies, was observed. Putative pathogenic or likely pathogenic monoallelic germline variants mapped to 10 cancer predisposition genes (CPGs: APC, CHEK2, DROSHA, ERCC5, FAH, MSH2, MUTYH, RPS19, TGFBR2 and VHL) were detected in 33% of the patients, only 40% of them with a family history of cancer. These findings showed a predominance of CPGs with a known link to gastrointestinal/colorectal and renal cancer risk. A remarkable feature was an enrichment of rare damaging variants affecting different classes of DNA repair genes, particularly those known as Fanconi anemia genes. Moreover, several potentially deleterious variants mapped to genes impacting liver functions were disclosed. To our knowledge, this is the largest assessment of rare germline variants in HB patients to date, contributing to elucidate the genetic architecture of HB risk.
    Keywords:  CYP1A1; DNA repair; ERCC5; MSH2; MUTYH; VHL; cancer predisposition; hepatoblastoma
    DOI:  https://doi.org/10.3389/fgene.2022.858396
  2. Am J Hum Genet. 2022 Apr 29. pii: S0002-9297(22)00155-0. [Epub ahead of print]
    Germline predisposition to pediatric Ewing sarcoma is characterized by inherited pathogenic variants in DNA damage repair genes.
    Riaz Gillani, Sabrina Y Camp, Seunghun Han, Jill K Jones, Hoyin Chu, Schuyler O'Brien, Erin L Young, Lucy Hayes, Gareth Mitchell, Trent Fowler, Alexander Gusev, Junne Kamihara, Katherine A Janeway, Joshua D Schiffman, Brian D Crompton, Saud H AlDubayan, Eliezer M Van Allen.
      More knowledge is needed regarding germline predisposition to Ewing sarcoma to inform biological investigation and clinical practice. Here, we evaluated the enrichment of pathogenic germline variants in Ewing sarcoma relative to other pediatric sarcoma subtypes, as well as patterns of inheritance of these variants. We carried out European-focused and pan-ancestry case-control analyses to screen for enrichment of pathogenic germline variants in 141 established cancer predisposition genes in 1,147 individuals with pediatric sarcoma diagnoses (226 Ewing sarcoma, 438 osteosarcoma, 180 rhabdomyosarcoma, and 303 other sarcoma) relative to identically processed cancer-free control individuals. Findings in Ewing sarcoma were validated with an additional cohort of 430 individuals, and a subset of 301 Ewing sarcoma parent-proband trios was analyzed for inheritance patterns of identified pathogenic variants. A distinct pattern of pathogenic germline variants was seen in Ewing sarcoma relative to other sarcoma subtypes. FANCC was the only gene with an enrichment signal for heterozygous pathogenic variants in the European Ewing sarcoma discovery cohort (three individuals, OR 12.6, 95% CI 3.0-43.2, p = 0.003, FDR = 0.40). This enrichment in FANCC heterozygous pathogenic variants was again observed in the European Ewing sarcoma validation cohort (three individuals, OR 7.0, 95% CI 1.7-23.6, p = 0.014), representing a broader importance of genes involved in DNA damage repair, which were also nominally enriched in individuals with Ewing sarcoma. Pathogenic variants in DNA damage repair genes were acquired through autosomal inheritance. Our study provides new insight into germline risk factors contributing to Ewing sarcoma pathogenesis.
    Keywords:  Ewing sarcoma, cancer predisposition, pediatric oncology, genetic risk
    DOI:  https://doi.org/10.1016/j.ajhg.2022.04.007
  3. Front Oncol. 2022 ;12 745796
    Germline Mutational Landscape in Chinese Patients With Advanced Breast Cancer.
    Jiayang Zhang, Nan Wang, Tiantian Zheng, Tan Lu, Ruyan Zhang, Ran Ran, Kun Li, Yong Huang, Feng Xie, Yue Zhang, Shidong Jia, Jianjun Yu, Huiping Li.
       Background: Genetic testing for breast cancer (BC) patients may shift the paradigm towards more personalized management and treatment strategies. While gene alterations may be ethnic-specific in breast cancer, our understanding of genetic epidemiology of BC remains mainly driven by data from Caucasian populations and further limited to selected handful of genes.
    Methods: We collected whole blood samples from 356 BC patients at metastatic first line BC and primary stage IV disease at Beijing Cancer Hospital between Jan. 2013 to Dec. 2019. A comprehensive 600-gene cancer panel was used to detect germline variants in the covered genes with a median 300x sequencing depth. Variants were classified into pathogenic, likely pathogenic, variant of uncertain significance, likely benign and benign groups according to the ACMG/AMP Standards and Guidelines. Pathogenic and likely pathogenic variants were considered as deleterious mutations.
    Results: The median age of 356 BC patients was 49 years (range, 21-87 years) at the first diagnosis of BC. Deleterious germline mutations across 48 cancer-related genes were identified in 21.6% (77/356) of the patients. The most prevalent mutations were BRCA1/2 mutations (7.0%), followed by ATM and RAD50 mutations (1.4% each). In addition, patients with family history were more likely to carry BRCA1 mutations (P=0.04). Moreover, patients with triple-negative breast cancer (TNBC) were more likely to harbor BRCA1 mutations than those with HR+ or HER2+ breast cancer (P=0.006). While there was no significant survival difference observed in BRCA1/2 carriers relative to non-carriers, patients with DNA damage repair (DDR) gene mutations (mostly frequently BRCA, ATM, RAD50) had worse disease-free survival (P=0.02).
    Conclusions: The most prevalent germline mutations in a large cohort of Chinese patients with advanced BC were BRCA1/2 mutations, followed by ATM and RAD50 mutations. In total, approximately 16.0% (57/356) of patients carry deleterious mutations in DDR pathway. Patients with breast or ovarian cancer family history were more likely to carry BRCA1/2 mutations, and ones with DDR mutations had worse survival. These findings suggest that DDR mutations are prevalent in Chinese BC patients who may potentially benefit from treatment with Poly (ADP-ribose) polymerase inhibitors.
    Keywords:  DNA-damage repair pathway; breast cancer; germline mutations; next-generation sequencing; prognosis
    DOI:  https://doi.org/10.3389/fonc.2022.745796
  4. Eur J Endocrinol. 2022 May 01. pii: EJE-21-0893. [Epub ahead of print]
    Convergence between germline and somatic mutations in pancreatic neuroendocrine tumors.
    Chao Ling, Xiafei Hong, Mengyue Xu, Yutong Wang, Xiaosen Ma, Yunying Cui, Rui Jiang, Dingyan Cao, Huanwen Wu, An-Li Tong, Yupei Zhao, Wenming Wu.
       OBJECTIVES: The pancreatic neuroendocrine tumors (PanNETs) are a group of clinically heterogeneous neoplasms. Although previous studies illustrated the somatic mutation pattern for PanNETs, the germline mutation pattern is still unclear. Here, we comprehensively screened the underlying germline mutations in a cohort of multiple endocrine neoplasia type 1 (MEN1)-related and sporadic PanNETs to reveal the characteristics of germline mutation in PanNET patients.
    METHODS: Patients diagnosed with PanNETs by biopsy or surgical pathology were enrolled in this study. Peripheral blood samples were used for genomic DNA purification and subsequent sequencing. The following sequencing techniques were used and compared for validation: 1) targeted gene capture with a customized panel; 2) whole exome sequencing data from previous study.
    RESULTS: A total of 184 PanNET patients were enrolled, including 20 MEN1-related and 164 sporadic cases. In this study, MEN1 mutation rate in MEN1-related PanNETs was 60% (12/20), of which 50% were novel mutation sites. For sporadic PanNETs, the overall germline mutation rate was very low. Besides the rare MEN1 mutation, previously unreported germline variant in DAXX was found in one non-functional PanNET.
    CONCLUSIONS: This study revealed distinctive germline mutation rates between MEN1-related and sporadic PanNETs. The novel MEN1 mutations contribute to revealing the spectrum of MEN1 mutations in PanNETs. The newly discovered germline variant of DAXX in sporadic PanNET implies a tendency of convergence between germline and somatic mutation genes.
    DOI:  https://doi.org/10.1530/EJE-21-0893
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