The NF90/NF45 Complex Participates in DNA Break Repair via Nonhomologous End Joining

Author:

Shamanna Raghavendra A.12,Hoque Mainul1,Lewis-Antes Anita1,Azzam Edouard I.32,Lagunoff David4,Pe'ery Tsafi15,Mathews Michael B.12

Affiliation:

1. Departments of Biochemistry and Molecular Biology, UMDNJ-New Jersey Medical School, UMDNJ, P.O. Box 1709, Newark, New Jersey 07101-1709

2. Graduate School of Biomedical Sciences, UMDNJ, P.O. Box 1709, Newark, New Jersey 07101-1709

3. Radiology, UMDNJ-New Jersey Medical School, UMDNJ, P.O. Box 1709, Newark, New Jersey 07101-1709

4. Surgery, UMDNJ-New Jersey Medical School, UMDNJ, P.O. Box 1709, Newark, New Jersey 07101-1709

5. Medicine, UMDNJ-New Jersey Medical School, UMDNJ, P.O. Box 1709, Newark, New Jersey 07101-1709

Abstract

ABSTRACT Nuclear factor 90 (NF90), an RNA-binding protein implicated in the regulation of gene expression, exists as a heterodimeric complex with NF45. We previously reported that depletion of the NF90/NF45 complex results in a multinucleated phenotype. Time-lapse microscopy revealed that binucleated cells arise by incomplete abscission of progeny cells followed by fusion. Multinucleate cells arose through aberrant division of binucleated cells and displayed abnormal metaphase plates and anaphase chromatin bridges suggestive of DNA repair defects. NF90 and NF45 are known to interact with the DNA-dependent protein kinase (DNA-PK), which is involved in telomere maintenance and DNA repair by nonhomologous end joining (NHEJ). We hypothesized that NF90 modulates the activity of DNA-PK. In an in vitro NHEJ assay system, DNA end joining was reduced by NF90/NF45 immunodepletion or by RNA digestion to an extent similar to that for catalytic subunit DNA-PKcs immunodepletion. In vivo , NF90/NF45-depleted cells displayed increased γ-histone 2A.X foci, indicative of an accumulation of double-strand DNA breaks (DSBs), and increased sensitivity to ionizing radiation consistent with decreased DSB repair. Further, NF90/NF45 knockdown reduced end-joining activity in vivo . These results identify the NF90/NF45 complex as a regulator of DNA damage repair mediated by DNA-PK and suggest that structured RNA may modulate this process.

Publisher

American Society for Microbiology

Subject

Cell Biology,Molecular Biology

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