Genetic variation in radiation-induced cell death.

Genome Res

Howard Hughes Medical Institute, University of Pennsylvania, Philadelphia, Pennsylvania 19104, USA.

Published: February 2012

AI Article Synopsis

  • Radiation exposure is common in various settings and while it can be harmful, it is also useful in treatments like cancer radiotherapy.
  • Understanding individual differences in how people respond to radiation is crucial for improving treatment efficacy and reducing risks.
  • By studying human cells, researchers identified genetic variants that affect how cells respond to radiation and pinpointed specific genes that could be targeted to enhance the effectiveness of radiation therapy in tumors.

Article Abstract

Radiation exposure through environmental, medical, and occupational settings is increasingly common. While radiation has harmful effects, it has utility in many applications such as radiotherapy for cancer. To increase the efficacy of radiation treatment and minimize its risks, a better understanding of the individual differences in radiosensitivity and the molecular basis of radiation response is needed. Here, we integrated human genetic and functional genomic approaches to study the response of human cells to radiation. We measured radiation-induced changes in gene expression and cell death in B cells from normal individuals. We found extensive individual variation in gene expression and cellular responses. To understand the genetic basis of this variation, we mapped the DNA sequence variants that influence expression response to radiation. We also identified radiation-responsive genes that regulate cell death; silencing of these genes by small interfering RNA led to an increase in radiation-induced cell death in human B cells, colorectal and prostate cancer cells. Together these results uncovered DNA variants that contribute to radiosensitivity and identified genes that can be targeted to increase the sensitivity of tumors to radiation.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3266040PMC
http://dx.doi.org/10.1101/gr.122044.111DOI Listing

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