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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.

Aberrant function of the C-terminal tail of HIST1H1E Aacelerates 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, M. E. Suzanne.; Meuwissen, Marije; Kenis, Sandra; Van der Aa, Nathalie; Larson, Austin; Brown, Kathleen; Wasserstein Melissa, P.; Skotko Brian, G.; Begtrup, Amber; Person, Richard; Karayiorgou, Maria; Roos J., Louw; Van Gassen Koen, L.; Koopmans, Marije; Bijlsma Emilia, K.; Santen Gijs, W. E.; Barge-Schaapveld Daniela, Q. C. M.; Ruivenkamp Claudia, A. L.; Hoffer Mariette, J. V.; Lalani Seema, R.; Streff, Haley; Craigen William, J.; Graham Brett, H.; van den Elzen Annette, P. M.; Kamphuis Daan, J.; Ounap, Katrin; Reinson, Karit; Pajusalu, Sander; Wojcik Monica, H.; Viberti, Clara; Di Gaetano, Cornelia; Bertini, Enrico; Petrucci, Simona; De Luca, Alessandro; Rota, Rossella; Ferretti, Elisabetta; Matullo, Giuseppe; Dallapiccola, Bruno; Sgura, Antonella; Walkiewicz, Magdalena; Kooy, R. Frank.; Tartaglia, Marco. - In: AMERICAN JOURNAL OF HUMAN GENETICS. - ISSN 0002-9297. - 105:3(2019), pp. 493-508. [10.1016/j.ajhg.2019.07.007]

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

Catanzaro Giuseppina;Miele Evelina;Petrucci Simona;Ferretti Elisabetta;
2019

Abstract

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.
2019
accelerated aging; cellular senescence; chromatin compaction; chromatin dynamics; chromatin remodeling; HIST1H1E; linker histone; linker histone H1.4; methylation profiling; replicative senescence; Aneuploidy; Cell Nucleolus; Cellular Senescence; Child; Chromatin; DNA Methylation; Female; Histones; Humans; Infant; Male; Middle Aged
01 Pubblicazione su rivista::01a Articolo in rivista
Aberrant function of the C-terminal tail of HIST1H1E Aacelerates 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, M. E. Suzanne.; Meuwissen, Marije; Kenis, Sandra; Van der Aa, Nathalie; Larson, Austin; Brown, Kathleen; Wasserstein Melissa, P.; Skotko Brian, G.; Begtrup, Amber; Person, Richard; Karayiorgou, Maria; Roos J., Louw; Van Gassen Koen, L.; Koopmans, Marije; Bijlsma Emilia, K.; Santen Gijs, W. E.; Barge-Schaapveld Daniela, Q. C. M.; Ruivenkamp Claudia, A. L.; Hoffer Mariette, J. V.; Lalani Seema, R.; Streff, Haley; Craigen William, J.; Graham Brett, H.; van den Elzen Annette, P. M.; Kamphuis Daan, J.; Ounap, Katrin; Reinson, Karit; Pajusalu, Sander; Wojcik Monica, H.; Viberti, Clara; Di Gaetano, Cornelia; Bertini, Enrico; Petrucci, Simona; De Luca, Alessandro; Rota, Rossella; Ferretti, Elisabetta; Matullo, Giuseppe; Dallapiccola, Bruno; Sgura, Antonella; Walkiewicz, Magdalena; Kooy, R. Frank.; Tartaglia, Marco. - In: AMERICAN JOURNAL OF HUMAN GENETICS. - ISSN 0002-9297. - 105:3(2019), pp. 493-508. [10.1016/j.ajhg.2019.07.007]
01a Articolo in rivista
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11573/1383117
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