Jump to content

Jan Karlseder

From Wikipedia, the free encyclopedia
(Redirected from Draft:Jan Karlseder)
Jan Karlseder
BornSeptember, 1968 (1968-09-23) (age 56)
Vienna, Austria
Alma materUniversity of Vienna
Known forDefining proliferative boundaries

Jan Karlseder (born September 28, 1968, in Innsbruck) an Austrian molecular biologist, is the Chief Science Officer[1] and a Senior Vice President at the Salk Institute for Biological Studies. He is also a professor in the Molecular and Cellular Biology Laboratory, the Director of the Paul F. Glenn Center for Biology of Aging Research[2] and the holder of the Donald and Darlene Shiley Chair at the Salk Institute for Biological Studies.

Career

[edit]

Karlseder obtained both his M.Sc. and his Ph.D. at the University of Vienna. In 1996, he joined the Laboratory of Titia de Lange at Rockefeller University in New York City for postdoctoral training. He became a faculty member at the Salk Institute for Biological Studies in 2002.[citation needed]

Research

[edit]

Karlseder discovered that telomere dysfunction plays a role in Werner Syndrome, a premature aging disease that is associated with early onset of cancer. WRN helicase, which is mutated in Werner Syndrome patients, is required for efficient replication of the telomeric G-strand.[3] Without WRN, lagging strand replication frequently stalls at telomeres, leading to loss of one of the sister telomeres during replication and cell division. This telomere loss in turn can lead to telomere end-to-end fusions, fusion-bridge-breakage cycles and genome instability, which is responsible for the heightened cancer incidence in individuals with Werner Syndrome.[4] He went on to show that following DNA replication telomeres are recognized by the intracellular DNA damage machinery.[5] This seemingly paradoxical event turned out to be essential to recruit the machinery that establishes protection at chromosome ends, where the homologous recombination machinery acts to form a structure that is resistant to nucleases and damage repair.[6]

Karlseder’s work on DNA repair pathway choice led to the discovery of the microprotein CYREN, which inhibits error prone non-homologous end-joining during S and G2 phases of the cell cycle, thereby promoting DNA break repair by the error free homologous recombination machinery.[7]

Karlseder discovered that mitotic arrest leads to telomere deprotection, which triggers a stress response that leads to the  death of cells that cannot complete mitosis. He demonstrated that this process is at play during replicative crisis, where fused telomeres trigger mitotic arrest and in turn cell death within one or two cell cycles.[8][9]

Karlseder’s work on recombination-based telomere maintenance (ALT) revealed that constitutive damage signals from shortening telomeres down-regulate histone synthesis, which leads to changes in nucleosome availability and histone chaperone expression.[10] This led to the discovery that replication fork stalling at telomeres plays a major role in the activation of ALT.[11]

He found that cell death in replicative crisis is executed by the autophagy machinery. Autophagy suppression allowed cells to bypass crisis and continue to proliferate with critically short telomeres, accumulating high levels of genome instability, pointing at autophagy as a potent tumor suppressor during the earliest stages of cancer initiation.[12]

Karlseder’s work on connecting telomere dysfunction with inflammation and cell death during replicative crisis identified ZBP1 as novel regulator of the innate RNA sensing machinery. He discovered that cells in replicative crisis use the telomeric transcript TERRA as messenger to sense critically short telomeres. TERRA associates with the innate RNA sensor ZBP1, which in turn forms filaments at the mitochondrial outer membrane, where it activates its adaptor MAVS, resulting in an amplification of an interferon type 1 inflammation response. Karlseder thereby discovered a novel tumor suppressive pathway, which removes aged cells with critically short telomeres, which would be prone to cancerous transformation.[13]

References

[edit]
  1. ^ "Executive Leadership Team". Salk Institute for Biological Studies. Retrieved 2024-02-13.
  2. ^ "Glenn Foundation for Medical Research Glenn Center for Research on Aging". glennfoundation.org. Retrieved 2021-01-20.
  3. ^ Crabbe, Laure; Verdun, Ramiro E.; Haggblom, Candy I.; Karlseder, Jan (2004-12-10). "Defective Telomere Lagging Strand Synthesis in Cells Lacking WRN Helicase Activity". Science. 306 (5703): 1951–1953. Bibcode:2004Sci...306.1951C. doi:10.1126/science.1103619. ISSN 0036-8075. PMID 15591207. S2CID 32602639.
  4. ^ Crabbe, L.; Jauch, A.; Naeger, C. M.; Holtgreve-Grez, H.; Karlseder, J. (2007-02-06). "Telomere dysfunction as a cause of genomic instability in Werner syndrome". Proceedings of the National Academy of Sciences. 104 (7): 2205–2210. Bibcode:2007PNAS..104.2205C. doi:10.1073/pnas.0609410104. ISSN 0027-8424. PMC 1794219. PMID 17284601.
  5. ^ Verdun, Ramiro E.; Crabbe, Laure; Haggblom, Candy; Karlseder, Jan (2005). "Functional Human Telomeres Are Recognized as DNA Damage in G2 of the Cell Cycle". Molecular Cell. 20 (4): 551–561. doi:10.1016/j.molcel.2005.09.024. PMID 16307919.
  6. ^ Verdun, Ramiro E.; Karlseder, Jan (2006). "The DNA Damage Machinery and Homologous Recombination Pathway Act Consecutively to Protect Human Telomeres". Cell. 127 (4): 709–720. doi:10.1016/j.cell.2006.09.034. PMID 17110331. S2CID 16644043.
  7. ^ Arnoult, Nausica; Correia, Adriana; Ma, Jiao; Merlo, Anna; Garcia-Gomez, Sara; Maric, Marija; Tognetti, Marco; Benner, Christopher W.; Boulton, Simon J.; Saghatelian, Alan; Karlseder, Jan (2017-09-20). "Regulation of DNA repair pathway choice in S and G2 phases by the NHEJ inhibitor CYREN". Nature. 549 (7673): 548–552. Bibcode:2017Natur.549..548A. doi:10.1038/nature24023. ISSN 1476-4687. PMC 5624508. PMID 28959974.
  8. ^ Hayashi, Makoto T.; Cesare, Anthony J.; Fitzpatrick, James A. J.; Lazzerini-Denchi, Eros; Karlseder, Jan (April 2012). "A telomere-dependent DNA damage checkpoint induced by prolonged mitotic arrest". Nature Structural & Molecular Biology. 19 (4): 387–394. doi:10.1038/nsmb.2245. ISSN 1545-9985. PMC 3319806. PMID 22407014.
  9. ^ Hayashi, Makoto T.; Cesare, Anthony J.; Rivera, Teresa; Karlseder, Jan (June 2015). "Cell death during crisis is mediated by mitotic telomere deprotection". Nature. 522 (7557): 492–496. Bibcode:2015Natur.522..492H. doi:10.1038/nature14513. ISSN 1476-4687. PMC 4481881. PMID 26108857.
  10. ^ O'Sullivan, Roderick J.; Kubicek, Stefan; Schreiber, Stuart L.; Karlseder, Jan (October 2010). "Reduced histone biosynthesis and chromatin changes arising from a damage signal at telomeres". Nature Structural & Molecular Biology. 17 (10): 1218–1225. doi:10.1038/nsmb.1897. ISSN 1545-9985. PMC 2951278. PMID 20890289.
  11. ^ O'Sullivan, Roderick J.; Arnoult, Nausica; Lackner, Daniel H.; Oganesian, Liana; Haggblom, Candy; Corpet, Armelle; Almouzni, Genevieve; Karlseder, Jan (February 2014). "Rapid induction of alternative lengthening of telomeres by depletion of the histone chaperone ASF1". Nature Structural & Molecular Biology. 21 (2): 167–174. doi:10.1038/nsmb.2754. ISSN 1545-9985. PMC 3946341. PMID 24413054.
  12. ^ Nassour, Joe; Radford, Robert; Correia, Adriana; Fusté, Javier Miralles; Schoell, Brigitte; Jauch, Anna; Shaw, Reuben J.; Karlseder, Jan (January 2019). "Autophagic cell death restricts chromosomal instability during replicative crisis". Nature. 565 (7741): 659–663. Bibcode:2019Natur.565..659N. doi:10.1038/s41586-019-0885-0. ISSN 1476-4687. PMC 6557118. PMID 30675059.
  13. ^ Nassour, Joe; Aguiar, Lucia Gutierrez; Correia, Adriana; Schmidt, Tobias T.; Mainz, Laura; Przetocka, Sara; Haggblom, Candy; Tadepalle, Nimesha; Williams, April; Shokhirev, Maxim N.; Akincilar, Semih C.; Tergaonkar, Vinay; Shadel, Gerald S.; Karlseder, Jan (2023-02-08). "Telomere-to-mitochondria signalling by ZBP1 mediates replicative crisis". Nature. 614 (7949): 767–773. Bibcode:2023Natur.614..767N. doi:10.1038/s41586-023-05710-8. ISSN 0028-0836. PMC 9946831. PMID 36755096.