Genetic mechanisms underlying sexual dimorphism in cancer and response to therapy

癌症性别二态性的遗传机制和治疗反应

• 批准号: 10204724
• 负责人: Rong Stephanie Huang
• 金额: --
• 依托单位: NORTHWESTERN UNIVERSITY AT CHICAGO
• 依托单位国家: 美国
• 财政年份: 2019
• 资助国家: 美国
• 起止时间: 2019-06-01 至 2025-05-31
• 项目状态: 未结题
• 来源: https://reporter.nih.gov/project-details/10204724
• 关键词: Affect; Age of Onset; Alleles; Allelic Imbalance; Awareness; Biological Models; Cancer Biology; Cancer cell line; Caring; Cell model; Characteristics; Clinical; Complex; DNA Methylation; Data; Diagnosis; Disease; Drug Modelings; Environmental Exposure; Epigenetic Process; Exhibits; Exons; Expenditure; Female; Gene Expression; Genes; Genetic; Genetic Models; Genetic Risk; Genetic Variation; Genomics; Goals; Hepatocyte; Heritability; Hormonal; Hormones; Human; Incidence; Individual; Inherited; Knowledge; Lead; Literature; Malignant Neoplasms; Mediating; Messenger RNA; MicroRNAs; Molecular; Morbidity - disease rate; Oncogenes; Pathway interactions; Patients; Penetrance; Pharmaceutical Preparations; Pharmacogenomics; Pharmacotherapy; Precision Medicine Initiative; Predisposition; Prognosis; Protocols documentation; Regulation; Research; Resources; Risk; Risk Factors; Sampling; Sex Chromosomes; Sex Differences; Somatic Mutation; System; Testing; The Cancer Genome Atlas; Therapeutic; Tumor-Derived; United States; Variant; Woman; Work; X Chromosome; Y Chromosome; base; cancer genome; cancer genomics; cancer risk; cancer therapy; computational pipelines; dimorphism; drug sensitivity; experience; gene therapy; genetic architecture; genetic risk factor; genetic variant; genome wide association study; improved outcome; in vitro Model; lymphoblastoid cell line; male; men; molecular phenotype; mortality; novel marker; precision medicine; predictive modeling; protective factors; response; sex; sexual dimorphism; targeted treatment; therapeutic target; trait; transcriptome; treatment response; tumor

PROJECT SUMMARY/ABSTRACT Cancer comprises a diverse group of diseases with significant morbidity and mortality. Nearly all common cancers exhibit some form of sexual dimorphism, for example in incidence, prognosis, or response to therapy. This dimorphism has been hypothesized to derive from differences between males and females in hormones, sex chromosomes, and environmental exposures; however the molecular basis of these disparities remains largely unknown. An understanding of this dimorphism is fundamental to precision medicine in cancer, and may lead to discovery of novel biomarkers, therapeutic targets, and improved outcomes. We propose to discover the molecular basis of sexual dimorphism in cancer though the following Aims: Aim 1 will characterize sexual dimorphism in gene expression and its regulation within and between tumor types of NCI's The Cancer Genome Atlas (TCGA). Leveraging TCGA, we will characterize sexual dimorphism at the transcriptome level and its potential genomic and epigenetic causes within and across cancers. Aim 2 will characterize sexual dimorphism in the heritable genetic component of cancer susceptibility across common cancers. Utilizing data from the largest genome-wide association studies of cancer we will search for differences in the genetic architecture between males and females. We determine what proportion of the heritable component of each cancer is shared across sexes, and also estimate how much sex-specific sharing across cancers. Using multiple genetic models, we will perform sex-aware association studies to identify genetic variants that affect males and females differently. We will test a model for genetic risk, whereby the same alleles affect both sexes, but the lower-risk sex would require more or stronger genetic risk factors to develop disease. We will test for specific risk or protective factors encoded on the sex chromosomes that affect the sexes differentially. We will test for gene-sex interactions whereby autosomal loci act in a sex-dependent manner, with or without hormonally-mediated or other sexual dimorphism acting at the gene expression level. Aim 3 will characterize sexual dimorphism in response to therapeutics and define the molecular features and mechanisms contributing to that dimorphism. Utilizing molecular and phenotypic drug response data from over 1000 cancer cell lines from the Cancer Genome Project (CGP), we will build sex- specific predictive models of drug response that we will then apply to gene expression data from the full set of TCGA tumor samples to impute a sex-specific drug response for each TCGA sample. We will correlate imputed drug responses to TCGA tumor molecular features, with focus on those identified in Aims 1 and 2 and candidates suggested by our preliminary data and the literature. We will functionally validate predicted sexually dimorphic response to therapy using cell models, including panels of lymphoblastoid cell lines, human hepatocytes, and cancer cell lines. The results of this study will define genetic and genomic features that underlie sexual dimorphism in cancer biology, susceptibility, and response to therapeutics.

项目总结/文摘