Word Cloud for Genetics Branch: instability, research, plasticity, alterability, heredity, variation, chromosomes, DNA, mutation, human genome, alleles, translation, screening, diagnostics, RNA, therapy, counseling, prevention, correlation, biomarkers.
Chief
Paul S. Meltzer, M.D., Ph.D.
Program Assistant
Nancy Dossa Sossavi

Center for Cancer Research
National Cancer Institute

Building 37, Room 6138
Bethesda, MD 20892-4265
301-496-5266

Among the defining concepts of the Genetics Branch is one that underlies its basic research focus and others that form the foundation of its clinical and translational research activities. The concept that underlies basic research is that cancer is a genetic disease caused by genetic instability. That instability is a function of all the inherited and acquired effects that mediate plasticity and alterability at the level of DNA. The success of molecular genetics over the past two decades has been the identification of genes involved in pathways of growth and development, and the identification of the mechanisms by which the normal regulation and/or products of these genes are altered in cancer. The elucidation of the necessary and sufficient factors that govern genetic instability, the description of the common and disparate themes among different types of instability, and the cataloging of distinct patterns of gene expression in tumors compared to the normal tissues from which they arise are within the purview and distinct perspective of this branch. There is, in addition, a clinical/translational mantle that this branch is called upon to shoulder.

At the clinical level this includes patient cancer risk screening, education, counseling, genetic testing (for those who choose to be tested, with testing provided in a setting that is attentive to all the ethical and legal aspects of the testing decision), and the development of appropriate surveillance and prevention options that take into account the category of risk that an individual patient, family, or population represents.

The translational research that supports this clinical enterprise consists of four components: (1) molecular diagnostics; (2) genotype/phenotype correlations; (3) the development of biomarkers that can be used for risk assessment and as intermediate endpoints for chemoprevention trials; and (4) targeted therapy and assays for active agents based on the underlying genetics and mechanism(s) of genetic instability that distinguish a tumor from the normal cells from which it arose. The Genetics Branch also is the site for the intramural NCI initiative to develop a repository and database for high-resolution FISH-mapped STS-tagged BAC clones spaced at 1-2 Mb intervals across the human and murine genomes. We hope that this repository and database will serve as a general resource to the entire biomedical community for exploration of cancer-specific chromosomal aberrations.

Link to Clinicaltrials.gov Protocol ID Referral Phone Physician

A Comprehensive Omics Analysis of Pediatric Oncology Solid Tumors and Establishment of a Repository for Related Biological Studies

NCI-10-C-0086 1-877-624-4878 Javed Khan, M.D.
Position Contact Name Contact E-mail Contact Phone Research Area Keywords Number of Positions
Postdoctoral Fellow Munira A. Basrai, Ph.D., Senior Investigator

basraim@nih.gov

301-402-2552

Chromosome segregation, cell cycle, mitosis

1

About

Among the defining concepts of the Genetics Branch is one that underlies its basic research focus and others that form the foundation of its clinical and translational research activities. The concept that underlies basic research is that cancer is a genetic disease caused by genetic instability. That instability is a function of all the inherited and acquired effects that mediate plasticity and alterability at the level of DNA. The success of molecular genetics over the past two decades has been the identification of genes involved in pathways of growth and development, and the identification of the mechanisms by which the normal regulation and/or products of these genes are altered in cancer. The elucidation of the necessary and sufficient factors that govern genetic instability, the description of the common and disparate themes among different types of instability, and the cataloging of distinct patterns of gene expression in tumors compared to the normal tissues from which they arise are within the purview and distinct perspective of this branch. There is, in addition, a clinical/translational mantle that this branch is called upon to shoulder.

At the clinical level this includes patient cancer risk screening, education, counseling, genetic testing (for those who choose to be tested, with testing provided in a setting that is attentive to all the ethical and legal aspects of the testing decision), and the development of appropriate surveillance and prevention options that take into account the category of risk that an individual patient, family, or population represents.

The translational research that supports this clinical enterprise consists of four components: (1) molecular diagnostics; (2) genotype/phenotype correlations; (3) the development of biomarkers that can be used for risk assessment and as intermediate endpoints for chemoprevention trials; and (4) targeted therapy and assays for active agents based on the underlying genetics and mechanism(s) of genetic instability that distinguish a tumor from the normal cells from which it arose. The Genetics Branch also is the site for the intramural NCI initiative to develop a repository and database for high-resolution FISH-mapped STS-tagged BAC clones spaced at 1-2 Mb intervals across the human and murine genomes. We hope that this repository and database will serve as a general resource to the entire biomedical community for exploration of cancer-specific chromosomal aberrations.

Clinical Trials

Link to Clinicaltrials.gov Protocol ID Referral Phone Physician

A Comprehensive Omics Analysis of Pediatric Oncology Solid Tumors and Establishment of a Repository for Related Biological Studies

NCI-10-C-0086 1-877-624-4878 Javed Khan, M.D.

Directory

Positions

Position Contact Name Contact E-mail Contact Phone Research Area Keywords Number of Positions
Postdoctoral Fellow Munira A. Basrai, Ph.D., Senior Investigator

basraim@nih.gov

301-402-2552

Chromosome segregation, cell cycle, mitosis

1