Nhp6, an HMG1 protein, functions in SNR6 transcription by RNA polymerase III in S. cerevisiae

Michael Kruppa; Robyn D. Moir; David Kolodrubetz; Ian M. Willis

doi:10.1016/S1097-2765(01)00179-4

Nhp6, an HMG1 protein, functions in SNR6 transcription by RNA polymerase III in S. cerevisiae

Michael Kruppa, Robyn D. Moir, David Kolodrubetz, Ian M. Willis

Biochemistry

Research output: Contribution to journal › Article › peer-review

63 Scopus citations

Abstract

Nhp6A and Nhp6B are HMG1-like proteins required for the growth of S. cerevisiae at elevated temperatures. We show that the conditional lethality of an nhp6 strain results from defective transcription of SNR6 (U6 snRNA) by RNA polymerase III. Overexpression of U6 snRNA or Brf1, a limiting component of TFIIIB, and an activating mutation (PCF1-1) in TFIIIC were each found to suppress the nhp6 growth defect. Additionally, U6 snRNA levels, which are reduced over 10-fold in nhp6 cells at 37°C, were restored by Brf1 overexpression and by PCF1-1. Nhp6A protein specifically enhanced TFIIIC-dependent, but not TATA box-dependent, SNR6 transcription in vitro by facilitating TFIIIC binding to the SNR6 promoter. Thus, Nhp6 has a direct role in transcription complex assembly at SNR6.

Original language	English (US)
Pages (from-to)	309-318
Number of pages	10
Journal	Molecular Cell
Volume	7
Issue number	2
DOIs	https://doi.org/10.1016/S1097-2765(01)00179-4
State	Published - 2001

ASJC Scopus subject areas

Molecular Biology
Cell Biology

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title = "Nhp6, an HMG1 protein, functions in SNR6 transcription by RNA polymerase III in S. cerevisiae",

abstract = "Nhp6A and Nhp6B are HMG1-like proteins required for the growth of S. cerevisiae at elevated temperatures. We show that the conditional lethality of an nhp6 strain results from defective transcription of SNR6 (U6 snRNA) by RNA polymerase III. Overexpression of U6 snRNA or Brf1, a limiting component of TFIIIB, and an activating mutation (PCF1-1) in TFIIIC were each found to suppress the nhp6 growth defect. Additionally, U6 snRNA levels, which are reduced over 10-fold in nhp6 cells at 37°C, were restored by Brf1 overexpression and by PCF1-1. Nhp6A protein specifically enhanced TFIIIC-dependent, but not TATA box-dependent, SNR6 transcription in vitro by facilitating TFIIIC binding to the SNR6 promoter. Thus, Nhp6 has a direct role in transcription complex assembly at SNR6.",

author = "Michael Kruppa and Moir, {Robyn D.} and David Kolodrubetz and Willis, {Ian M.}",

note = "Funding Information: This research was supported by NIH grants GM45793 (D. K.) and GM42728 (I. M. W.). M. K. was supported in part by NIH training grant T32-AI-07271.",

year = "2001",

doi = "10.1016/S1097-2765(01)00179-4",

language = "English (US)",

volume = "7",

pages = "309--318",

journal = "Molecular Cell",

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T1 - Nhp6, an HMG1 protein, functions in SNR6 transcription by RNA polymerase III in S. cerevisiae

AU - Kruppa, Michael

AU - Moir, Robyn D.

AU - Kolodrubetz, David

AU - Willis, Ian M.

N1 - Funding Information: This research was supported by NIH grants GM45793 (D. K.) and GM42728 (I. M. W.). M. K. was supported in part by NIH training grant T32-AI-07271.

PY - 2001

Y1 - 2001

N2 - Nhp6A and Nhp6B are HMG1-like proteins required for the growth of S. cerevisiae at elevated temperatures. We show that the conditional lethality of an nhp6 strain results from defective transcription of SNR6 (U6 snRNA) by RNA polymerase III. Overexpression of U6 snRNA or Brf1, a limiting component of TFIIIB, and an activating mutation (PCF1-1) in TFIIIC were each found to suppress the nhp6 growth defect. Additionally, U6 snRNA levels, which are reduced over 10-fold in nhp6 cells at 37°C, were restored by Brf1 overexpression and by PCF1-1. Nhp6A protein specifically enhanced TFIIIC-dependent, but not TATA box-dependent, SNR6 transcription in vitro by facilitating TFIIIC binding to the SNR6 promoter. Thus, Nhp6 has a direct role in transcription complex assembly at SNR6.

AB - Nhp6A and Nhp6B are HMG1-like proteins required for the growth of S. cerevisiae at elevated temperatures. We show that the conditional lethality of an nhp6 strain results from defective transcription of SNR6 (U6 snRNA) by RNA polymerase III. Overexpression of U6 snRNA or Brf1, a limiting component of TFIIIB, and an activating mutation (PCF1-1) in TFIIIC were each found to suppress the nhp6 growth defect. Additionally, U6 snRNA levels, which are reduced over 10-fold in nhp6 cells at 37°C, were restored by Brf1 overexpression and by PCF1-1. Nhp6A protein specifically enhanced TFIIIC-dependent, but not TATA box-dependent, SNR6 transcription in vitro by facilitating TFIIIC binding to the SNR6 promoter. Thus, Nhp6 has a direct role in transcription complex assembly at SNR6.

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SN - 1097-2765

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JO - Molecular Cell

JF - Molecular Cell

IS - 2

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Nhp6, an HMG1 protein, functions in SNR6 transcription by RNA polymerase III in S. cerevisiae

Abstract

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