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PubMed ID   23713010 Publish Date   2013 May
Journal   Commun Integr Biol Species   Homo sapiens
Disease Type   Technology  
Title   Mitotic errors, aneuploidy and micronuclei in Hodgkin lymphoma pathogenesis
Authors   Maxwel M. Krem1, Marshall S. Horwitz
Affiliation   Department of Medicine; Institute for Stem Cell and Regenerative Medicine; University of Washington School of Medicine; Seattle, WA USA
Chromothripsis Definition   Close-by breakpoints: NA
Copy number states: NA
Fragments random joining: NA
Abstract   The Reed-Sternberg (RS) cell is the driving force behind Hodgkin lymphoma (HL), a unique malignancy in which the rare RS cell creates an inflammatory microenvironment that recruits a reactive tumor infiltrate. Well-known oncogenic factors such as nuclear factor kappa B (NFkappaB) signaling and Epstein-Barr virus infection are linked to HL pathogenesis but do not adequately explain the RS cell's key pathologic features of multi-nucleation, abnormalities of centrosome function and number and aneuploidy. Chromosomal instability is also considered a key pathway in the origin of the RS cell, though the molecular mechanisms have largely been a black box. We demonstrated that the midbody kelch domain protein KLHDC8B protects against mitotic errors, centrosomal amplification and chromosomal instability. Here we discuss how the new findings linking KLHDC8B to mitoticintegrity and faithful chromosomal segregation are providing mechanistic explanations for the origin of the RS cell and the molecular pathogenesis of chromosomal instability in HL.
 
 
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