Transcription elongation defects link oncogenic SF3B1 mutations to targetable alterations in chromatin landscape

Prajwal C. Boddu; Abhishek K. Gupta; Rahul Roy; Bárbara De La Peña Avalos; Anne Olazabal-Herrero; Nils Neuenkirchen; Joshua T. Zimmer; Namrata S. Chandhok; Darren King; Yasuhito Nannya; Seishi Ogawa; Haifan Lin; Matthew D. Simon; Eloise Dray; Gary M. Kupfer; Amit Verma; Karla M. Neugebauer; Manoj M. Pillai

doi:10.1016/j.molcel.2024.02.032

Transcription elongation defects link oncogenic SF3B1 mutations to targetable alterations in chromatin landscape

Prajwal C. Boddu
, Abhishek K. Gupta
, Rahul Roy
, Bárbara De La Peña Avalos
, Anne Olazabal-Herrero
, Nils Neuenkirchen
, Joshua T. Zimmer
, Namrata S. Chandhok
, Darren King
, Yasuhito Nannya
, Seishi Ogawa
, Haifan Lin
, Matthew D. Simon
, Eloise Dray
, Gary M. Kupfer
, Amit Verma
, Karla M. Neugebauer
, Manoj M. Pillai

Producción científica: Article › revisión exhaustiva

20 Citas (Scopus)

Resumen

Transcription and splicing of pre-messenger RNA are closely coordinated, but how this functional coupling is disrupted in human diseases remains unexplored. Using isogenic cell lines, patient samples, and a mutant mouse model, we investigated how cancer-associated mutations in SF3B1 alter transcription. We found that these mutations reduce the elongation rate of RNA polymerase II (RNAPII) along gene bodies and its density at promoters. The elongation defect results from disrupted pre-spliceosome assembly due to impaired protein-protein interactions of mutant SF3B1. The decreased promoter-proximal RNAPII density reduces both chromatin accessibility and H3K4me3 marks at promoters. Through an unbiased screen, we identified epigenetic factors in the Sin3/HDAC/H3K4me pathway, which, when modulated, reverse both transcription and chromatin changes. Our findings reveal how splicing factor mutant states behave functionally as epigenetic disorders through impaired transcription-related changes to the chromatin landscape. We also present a rationale for targeting the Sin3/HDAC complex as a therapeutic strategy.

Idioma original	English (US)
Páginas (desde-hasta)	1475-1495.e18
Publicación	Molecular Cell
Volumen	84
N.º	8
DOI	https://doi.org/10.1016/j.molcel.2024.02.032
Estado	Published - abr 18 2024

ASJC Scopus subject areas

Molecular Biology
Cell Biology

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10.1016/j.molcel.2024.02.032

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Boddu, P. C., Gupta, A. K., Roy, R., De La Peña Avalos, B., Olazabal-Herrero, A., Neuenkirchen, N., Zimmer, J. T., Chandhok, N. S., King, D., Nannya, Y., Ogawa, S., Lin, H., Simon, M. D., Dray, E., Kupfer, G. M., Verma, A., Neugebauer, K. M., & Pillai, M. M. (2024). Transcription elongation defects link oncogenic SF3B1 mutations to targetable alterations in chromatin landscape. Molecular Cell, 84(8), 1475-1495.e18. https://doi.org/10.1016/j.molcel.2024.02.032

Boddu, PC, Gupta, AK, Roy, R, De La Peña Avalos, B, Olazabal-Herrero, A, Neuenkirchen, N, Zimmer, JT, Chandhok, NS, King, D, Nannya, Y, Ogawa, S, Lin, H, Simon, MD, Dray, E, Kupfer, GM, Verma, A, Neugebauer, KM & Pillai, MM 2024, 'Transcription elongation defects link oncogenic SF3B1 mutations to targetable alterations in chromatin landscape', Molecular Cell, vol. 84, n.º 8, pp. 1475-1495.e18. https://doi.org/10.1016/j.molcel.2024.02.032

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title = "Transcription elongation defects link oncogenic SF3B1 mutations to targetable alterations in chromatin landscape",

abstract = "Transcription and splicing of pre-messenger RNA are closely coordinated, but how this functional coupling is disrupted in human diseases remains unexplored. Using isogenic cell lines, patient samples, and a mutant mouse model, we investigated how cancer-associated mutations in SF3B1 alter transcription. We found that these mutations reduce the elongation rate of RNA polymerase II (RNAPII) along gene bodies and its density at promoters. The elongation defect results from disrupted pre-spliceosome assembly due to impaired protein-protein interactions of mutant SF3B1. The decreased promoter-proximal RNAPII density reduces both chromatin accessibility and H3K4me3 marks at promoters. Through an unbiased screen, we identified epigenetic factors in the Sin3/HDAC/H3K4me pathway, which, when modulated, reverse both transcription and chromatin changes. Our findings reveal how splicing factor mutant states behave functionally as epigenetic disorders through impaired transcription-related changes to the chromatin landscape. We also present a rationale for targeting the Sin3/HDAC complex as a therapeutic strategy.",

keywords = "DNA damage response, R-loops, RNA polymerase II, SF3B1, Sin3/HDAC, U2AF1, WDR5, co-transcriptional splicing, spliceosome, transcription",

author = "Boddu, \{Prajwal C.\} and Gupta, \{Abhishek K.\} and Rahul Roy and \{De La Pe{\~n}a Avalos\}, B{\'a}rbara and Anne Olazabal-Herrero and Nils Neuenkirchen and Zimmer, \{Joshua T.\} and Chandhok, \{Namrata S.\} and Darren King and Yasuhito Nannya and Seishi Ogawa and Haifan Lin and Simon, \{Matthew D.\} and Eloise Dray and Kupfer, \{Gary M.\} and Amit Verma and Neugebauer, \{Karla M.\} and Pillai, \{Manoj M.\}",

note = "Publisher Copyright: {\textcopyright} 2024 Elsevier Inc.",

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doi = "10.1016/j.molcel.2024.02.032",

language = "English (US)",

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T1 - Transcription elongation defects link oncogenic SF3B1 mutations to targetable alterations in chromatin landscape

AU - Boddu, Prajwal C.

AU - Gupta, Abhishek K.

AU - Roy, Rahul

AU - De La Peña Avalos, Bárbara

AU - Olazabal-Herrero, Anne

AU - Neuenkirchen, Nils

AU - Zimmer, Joshua T.

AU - Chandhok, Namrata S.

AU - King, Darren

AU - Nannya, Yasuhito

AU - Ogawa, Seishi

AU - Lin, Haifan

AU - Simon, Matthew D.

AU - Dray, Eloise

AU - Kupfer, Gary M.

AU - Verma, Amit

AU - Neugebauer, Karla M.

AU - Pillai, Manoj M.

PY - 2024/4/18

Y1 - 2024/4/18

N2 - Transcription and splicing of pre-messenger RNA are closely coordinated, but how this functional coupling is disrupted in human diseases remains unexplored. Using isogenic cell lines, patient samples, and a mutant mouse model, we investigated how cancer-associated mutations in SF3B1 alter transcription. We found that these mutations reduce the elongation rate of RNA polymerase II (RNAPII) along gene bodies and its density at promoters. The elongation defect results from disrupted pre-spliceosome assembly due to impaired protein-protein interactions of mutant SF3B1. The decreased promoter-proximal RNAPII density reduces both chromatin accessibility and H3K4me3 marks at promoters. Through an unbiased screen, we identified epigenetic factors in the Sin3/HDAC/H3K4me pathway, which, when modulated, reverse both transcription and chromatin changes. Our findings reveal how splicing factor mutant states behave functionally as epigenetic disorders through impaired transcription-related changes to the chromatin landscape. We also present a rationale for targeting the Sin3/HDAC complex as a therapeutic strategy.

AB - Transcription and splicing of pre-messenger RNA are closely coordinated, but how this functional coupling is disrupted in human diseases remains unexplored. Using isogenic cell lines, patient samples, and a mutant mouse model, we investigated how cancer-associated mutations in SF3B1 alter transcription. We found that these mutations reduce the elongation rate of RNA polymerase II (RNAPII) along gene bodies and its density at promoters. The elongation defect results from disrupted pre-spliceosome assembly due to impaired protein-protein interactions of mutant SF3B1. The decreased promoter-proximal RNAPII density reduces both chromatin accessibility and H3K4me3 marks at promoters. Through an unbiased screen, we identified epigenetic factors in the Sin3/HDAC/H3K4me pathway, which, when modulated, reverse both transcription and chromatin changes. Our findings reveal how splicing factor mutant states behave functionally as epigenetic disorders through impaired transcription-related changes to the chromatin landscape. We also present a rationale for targeting the Sin3/HDAC complex as a therapeutic strategy.

KW - DNA damage response

KW - R-loops

KW - RNA polymerase II

KW - SF3B1

KW - Sin3/HDAC

KW - U2AF1

KW - WDR5

KW - co-transcriptional splicing

KW - spliceosome

KW - transcription

UR - https://www.scopus.com/pages/publications/85189452931

UR - https://www.scopus.com/pages/publications/85189452931#tab=citedBy

U2 - 10.1016/j.molcel.2024.02.032

DO - 10.1016/j.molcel.2024.02.032

M3 - Article

C2 - 38521065

AN - SCOPUS:85189452931

SN - 1097-2765

VL - 84

SP - 1475-1495.e18

JO - Molecular Cell

JF - Molecular Cell

IS - 8

ER -

Transcription elongation defects link oncogenic SF3B1 mutations to targetable alterations in chromatin landscape

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