Attenuated DNA damage repair by trichostatin A through BRCA1 suppression

Y Zhang, T Carr, A Dimtchev, N Zaer… - Radiation …, 2007 - meridian.allenpress.com
Y Zhang, T Carr, A Dimtchev, N Zaer, A Dritschilo, M Jung
Radiation research, 2007meridian.allenpress.com
Abstract Zhang, Y., Carr, T., Dimtchev, A., Zaer, N., Dritschilo, A. and Jung, M. Attenuated
DNA Damage Repair by Trichostatin A through BRCA1 Suppression. Radiat. Res. 168, 115–
124 (2007). Recent studies have demonstrated that some histone deacetylase (HDAC)
inhibitors enhance cellular radiation sensitivity. However, the underlying mechanism for
such a radiosensitizing effect remains unexplored. Here we show evidence that treatment
with the HDAC inhibitor trichostatin A (TSA) impairs radiation-induced repair of DNA …
Abstract
Zhang, Y., Carr, T., Dimtchev, A., Zaer, N., Dritschilo, A. and Jung, M. Attenuated DNA Damage Repair by Trichostatin A through BRCA1 Suppression. Radiat. Res. 168, 115–124 (2007).
Recent studies have demonstrated that some histone deacetylase (HDAC) inhibitors enhance cellular radiation sensitivity. However, the underlying mechanism for such a radiosensitizing effect remains unexplored. Here we show evidence that treatment with the HDAC inhibitor trichostatin A (TSA) impairs radiation-induced repair of DNA damage. The effect of TSA on the kinetics of DNA damage repair was measured by performing the comet assay and γ-H2AX focus analysis in radioresistant human squamous carcinoma cells (SQ-20B). TSA exposure increased the amount of radiation-induced DNA damage and slowed the repair kinetics. Gene expression profiling also revealed that a majority of the genes that control cell cycle, DNA replication and damage repair processes were down-regulated after TSA exposure, including BRCA1. The involvement of BRCA1 was further demonstrated by expressing ectopic wild-type BRCA1 in a BRCA1 null cell line (HCC-1937). TSA treatment enhanced radiation sensitivity of HCC-1937/wtBRCA1 clonal cells, which restored cellular radiosensitivity (D0 = 1.63 Gy), to the control level (D0 = 1.03 Gy). However, TSA had no effect on the level of radiosensitivity of BRCA1 null cells. Our data demonstrate for the first time that TSA treatment modulates the radiation-induced DNA damage repair process, in part by suppressing BRCA1 gene expression, suggesting that BRCA1 is one of molecular targets of TSA.
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