Site-directed biochemical analyses reveal that the switchable C-terminus of Rpc31 contributes to RNA polymerase III transcription initiation

Author:

Shekhar Arvind Chandra1,Sun Yuan-En1,Khoo Seok-Kooi1,Lin Yu-Chun1,Malau Ester Betaria1,Chang Wei-Hau2,Chen Hung-Ta1ORCID

Affiliation:

1. Institute of Molecular Biology, Academia Sinica , Taipei , Taiwan , R.O.C

2. Institute of Chemistry, Academia Sinica , Taiwan , R.O.C

Abstract

Abstract Rpc31 is a subunit in the TFIIE-related Rpc82/34/31 heterotrimeric subcomplex of Saccharomyces cerevisiae RNA polymerase III (pol III). Structural analyses of pol III have indicated that the N-terminal region of Rpc31 anchors on Rpc82 and further interacts with the polymerase core and stalk subcomplex. However, structural and functional information for the C-terminal region of Rpc31 is sparse. We conducted a mutational analysis on Rpc31, which uncovered a functional peptide adjacent to the highly conserved Asp-Glu-rich acidic C-terminus. This C-terminal peptide region, termed ‘pre-acidic’, is important for optimal cell growth, tRNA synthesis, and stable association of Rpc31 in the pre-initiation complex (PIC). Our site-directed photo-cross-linking to map protein interactions within the PIC reveal that this pre-acidic region specifically targets Rpc34 during transcription initiation, but also interacts with the DNA entry surface in free pol III. Thus, we have uncovered a switchable Rpc31 C-terminal region that functions in an initiation-specific protein interaction for pol III transcription.

Funder

Ministry of Science and Technology

Academia Sinica

Publisher

Oxford University Press (OUP)

Subject

Genetics

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