Multiple protein-protein interactions converging on the Prp38 protein during 
activation of the human spliceosome.

Schütze, T.; Ulrich, A. K. C.; Apelt, L.; Will, C. L.; Bartlick, N.; Seeger, M.; Weber, G.; Lührmann, R.; Stelzl, U.; Wahl, M. C.

doi:10.1261/rna.054296.115

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Journal Article

Multiple protein-protein interactions converging on the Prp38 protein during activation of the human spliceosome.

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Will, C. L.
Department of Cellular Biochemistry, MPI for biophysical chemistry, Max Planck Society;

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Lührmann, R.
Department of Cellular Biochemistry, MPI for biophysical chemistry, Max Planck Society;

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Citation

Schütze, T., Ulrich, A. K. C., Apelt, L., Will, C. L., Bartlick, N., Seeger, M., et al. (2016). Multiple protein-protein interactions converging on the Prp38 protein during activation of the human spliceosome. RNA, 22(2), 265-277. doi:10.1261/rna.054296.115.

Cite as: https://hdl.handle.net/11858/00-001M-0000-0029-C3C3-9

Abstract

Spliceosomal Prp38 proteins contain a conserved amino-terminal domain, but only higher eukaryotic orthologs also harbor a carboxy-terminal RS domain, a hallmark of splicing regulatory SR proteins. We show by crystal structure analysis that the amino-terminal domain of human Prp38 is organized around three pairs of antiparallel alpha-helices and lacks similarities to RNA binding domains found in canonical SR proteins. Instead, yeast two-hybrid analyses suggest that the amino-terminal domain is a versatile protein protein interaction hub that possibly binds 12 other spliceosomal proteins, most of which are recruited at the same stage. as Prp38. By quantitative, alanine surface-scanning two-hybrid screens and biochemical analyses we delineated four distinct interfaces on the Prp38 amino-terminal domain. In vitro interaction assays using recombinant proteins showed that Prp38 can bind at least two proteins simultaneously via two different interfaces. Addition of excess Prp38 amino-terminal domain to in vitro splicing assays, but not of an interaction-deficient mutant, stalled splicing at a precatalytic stage. Our results show that human Prp38 is an unusual SR protein, whose amino-terminal domain is a multi-interface protein protein interaction platform that might organize the relative positioning of other proteins during splicing.