Quantitative Proteome
Analysis Reveals RNA Processing
Factors As Modulators of Ionizing Radiation-Induced Apoptosis in the <i>C. elegans</i> Germline.
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Abstract
The nematode <i>Caenorhabditis elegans</i> is an organism most recognized for forward and reverse
genetic and functional genomic approaches. Proteomic analyses of DNA
damage-induced apoptosis have not been shown because of a limited
number of cells undergoing apoptosis. We applied mass spectrometry-based
quantitative proteomics to evaluate protein changes induced by ionizing
radiation (IR) in isolated <i>C. elegans</i> germlines.
For this purpose, we used isobaric peptide termini labeling (IPTL)
combined with the data analysis tool IsobariQ, which utilizes MS/MS
spectra for relative quantification of peak pairs formed during fragmentation.
Using stringent statistical critera, we identified 48 proteins to
be significantly up- or down-regulated, most of which are part of
a highly interconnected protein–protein interaction network
dominated by proteins involved in translational control. RNA-mediated
depletion of a selection of the IR-regulated proteins revealed that
the conserved CAR-1/CGH-1/CEY-3 germline RNP complex acts as a novel
negative regulator of DNA-damage induced apoptosis. Finally, a central
role of nucleolar proteins in orchestrating these responses was confirmed
as the H/ACA snRNP protein GAR-1 was required for IR-induced apoptosis
in the <i>C. elegans</i> germline