Aberrant function of the C-terminal tail of HIST1H1E accelerates cellular senescence and causes premature aging

Flex, Elisabetta

Martinelli, Simone

Van Dijck, Anke

Ciolfi, Andrea

Cecchetti, Serena

Coluzzi, Elisa

Pannone, Luca

Andreoli, Cristina

Radio, Francesca Clementina

Pizzi, Simone

Carpentieri, Giovanna

Bruselles, Alessandro

Catanzaro, Giuseppina

Pedace, Lucia

Miele, Evelina

Carcarino, Elena

Ge, Xiaoyan

Chijiwa, Chieko

Lewis, Me Suzanne

Meuwissen, Marije

Histones mediate dynamic packaging of nuclear DNA in chromatin, a process that is precisely controlled to guarantee efficient compaction of the genome and proper chromosomal segregation during cell division and to accomplish DNA replication, transcription, and repair. Due to the important structural and regulatory roles played by histones, it is not surprising that histone functional dysregulation or aberrant levels of histones can have severe consequences for multiple cellular processes and ultimately might affect development or contribute to cell transformation. Recently, germline frameshift mutations involving the C-terminal tail of HIST1H1E, which is a widely expressed member of the linker histone family and facilitates higher-order chromatin folding, have been causally linked to an as-yet poorly defined syndrome that includes intellectual disability. We report that these mutations result in stable proteins that reside in the nucleus, bind to chromatin, disrupt proper compaction of DNA, and are associated with a specific methylation pattern. Cells expressing these mutant proteins have a dramatically reduced proliferation rate and competence, hardly enter into the S phase, and undergo accelerated senescence. Remarkably, clinical assessment of a relatively large cohort of subjects sharing these mutations revealed a premature aging phenotype as a previously unrecognized feature of the disorder. Our findings identify a direct link between aberrant chromatin remodeling, cellular senescence, and accelerated aging.

English

The American journal of human genetics / American Society of Human Genetics [Bethesda, Md] - New York, N.Y., 1949, currens

New York, N.Y. : 2019

0002-9297 [print]

1537-6605 [online]

10.1016/J.AJHG.2019.07.007

105 :3 (2019) , p. 493-508

000484435700005

31447100

https://doi.org/10.1016/J.AJHG.2019.07.007

https://repository.uantwerpen.be/docman/iruaauth/484a44/162533.pdf

Faculty of Medicine and Health Sciences 

Faculty of Pharmaceutical, Biomedical and Veterinary Sciences . Biomedical Sciences 

A1 Journal article 

Biology 

Human medicine 

Publications with a UAntwerp address

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https://hdl.handle.net/10067/1625330151162165141