David Pellman

David Pellman, M.D.

Margaret M. Dyson Professor of Pediatric Oncology (Dana-Farber Cancer Institute)
Professor of Cell Biology (HMS)
HHMI Investigator

David Pellman, M.D. is the Margaret M. Dyson Professor of Pediatric Oncology at the Dana-Farber Cancer Institute, a Professor of Cell Biology at Harvard Medical School, an Investigator of the Howard Hughes Medical Institute, and the Associate Director for Basic Science at the Dana-Farber/Harvard Cancer Center.  He received his undergraduate and medical degrees from the University of Chicago.  During medical school, he did research at the Rockefeller University.  His postdoctoral fellowship was at the Whitehead Institute/Massachusetts Institute of Technology.

The Pellman Lab works on the mechanism of cell division and how certain cell division errors drive rapid genome evolution.  The normal processes studied in the laboratory have included spindle positioning and asymmetric cell division, the mechanism of spindle assembly and cytokinesis, and the mechanism of nuclear envelope assembly and how it is coordinated with chromosome segregation.  The mutational processes studied in David’s group are particularly important for cancer, but have relevance for genome evolution in other contexts.  Current projects include: the mechanism of a newly discovered mutational process called “chromothripsis”, how the architecture and integrity of the nuclear envelope impacts genome maintenance, and the role of cytoplasmic chromatin in triggering innate immune proinflammatory signaling. The lab uses a variety of approaches which include, molecular genetics, biochemistry, and imaging.  Currently there is a heavy emphasis on using a combination of live-cell imaging and single-cell genome sequencing developed in the lab (“Look-Seq”) to relate the consequences of cell division errors to genome alterations. 

Dana Farber Cancer Institute

Dept. of Pediatrics, Mayer-612

450 Brookline Ave

Boston, MA 02115

Lab phone: 617-632-4918

Lab fax: 617-632-5363

Trisomy of a Down Syndrome Critical Region Globally Amplifies Transcription via HMGN1 Overexpression.
Authors: Authors: Mowery CT, Reyes JM, Cabal-Hierro L, Higby KJ, Karlin KL, Wang JH, Kimmerling RJ, Cejas P, Lim K, Li H, Furusawa T, Long HW, Pellman D, Chapuy B, Bustin M, Manalis SR, Westbrook TF, Lin CY, Lane AA.
Cell Rep
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TRPS1 Is a Lineage-Specific Transcriptional Dependency in Breast Cancer.
Authors: Authors: Witwicki RM, Ekram MB, Qiu X, Janiszewska M, Shu S, Kwon M, Trinh A, Frias E, Ramadan N, Hoffman G, Yu K, Xie Y, McAllister G, McDonald R, Golji J, Schlabach M, deWeck A, Keen N, Chan HM, Ruddy D, Rejtar T, Sovath S, Silver S, Sellers WR, Jagani Z, Hogarty MD, Roberts C, Brown M, Stegmaier K, Long H, Shivdasani RA, Pellman D, Polyak K.
Cell Rep
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Nuclear envelope assembly defects link mitotic errors to chromothripsis.
Authors: Authors: Liu S, Kwon M, Mannino M, Yang N, Renda F, Khodjakov A, Pellman D.
Nature
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Over-elongation of centrioles in cancer promotes centriole amplification and chromosome missegregation.
Authors: Authors: Marteil G, Guerrero A, Vieira AF, de Almeida BP, Machado P, Mendonça S, Mesquita M, Villarreal B, Fonseca I, Francia ME, Dores K, Martins NP, Jana SC, Tranfield EM, Barbosa-Morais NL, Paredes J, Pellman D, Godinho SA, Bettencourt-Dias M.
Nat Commun
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Cell Biology: When Your Own Chromosomes Act like Foreign DNA.
Authors: Authors: Spektor A, Umbreit NT, Pellman D.
Curr Biol
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Cancer biology: Genome jail-break triggers lockdown.
Authors: Authors: Umbreit NT, Pellman D.
Nature
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A Tubulin Binding Switch Underlies Kip3/Kinesin-8 Depolymerase Activity.
Authors: Authors: Arellano-Santoyo H, Geyer EA, Stokasimov E, Chen GY, Su X, Hancock W, Rice LM, Pellman D.
Dev Cell
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The EMT regulator ZEB2 is a novel dependency of human and murine acute myeloid leukemia.
Authors: Authors: Li H, Mar BG, Zhang H, Puram RV, Vazquez F, Weir BA, Hahn WC, Ebert B, Pellman D.
Blood
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How the Genome Folds, Divides, Lives, and Dies.
Authors: Authors: Johnson WL, Xie KT, Kwon M, Liu S, Pellman D.
Cold Spring Harb Symp Quant Biol
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Modeling the initiation of Ewing sarcoma tumorigenesis in differentiating human embryonic stem cells.
Authors: Authors: Gordon DJ, Motwani M, Pellman D.
Oncogene
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