Sara Buhrlage

Sara Buhrlage, Ph.D.

Associate Professor of Biological Chemistry and Molecular Pharmacology

617-632-1963

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Publications

The mission of our group is to develop first-in-class inhibitors and prototype drugs for DUBs that can be utilized to pharmacologically validate members of the gene family as new targets for cancer treatment and other diseases.

Research:

Degradation of cancer causing proteins

The number of biologically validated cancer drug targets far outnumbers the number of pharmacologically and clinically validated drug targets. A large reason for this disparity is that many cancer targets require modulation of protein-protein interactions typically considerable ‘undruggable.' To address this problem we identify novel targets and compounds that promote specific degradation of such targets. Proteins are tagged for degradation post-translationally by the addition of ubiquitin chains, which encode for proteosomal and lysosomal degradation. Addition and removal of ubiquitin tags on substrates are coordinated by the action of ubiquitin activating, conjugating, and ligating enzymes (E1, E2, E3) and deubiquitylating enzymes (DUB). A growing number of DUB family members have been shown to rescue oncoproteins from degradation using genetic methods however a lack of potent and selective small molecule inhibitors has hindered pharmacological and clinical validation of DUBs. DUBs are proteases, a class of enzymes for which clinical stage inhibitors of non-DUB members exist. The mission of our group is to develop first-in-class inhibitors and prototype drugs for DUBs that can be utilized to pharmacologically validate members of the gene family as new targets for cancer treatment and other diseases. Our approach is to: 1) Execute target, gene family and peptidomimetic approaches to achieve new DUB inhibitors; 2) Screen DUB inhibitor libraries for anti-cancer activities; and 3) Pursue validation and mechanistic work for selected DUBs and compounds. We are also committed to developing technologies that accelerate ubiquitin system and especially DUB research. To accomplish these goals we work as a collaborative team of synthetic chemists, biochemists, cell biologists and structural biologists.

Address:

Dana-Farber Cancer Institute

Longwood Center-3311

450 Brookline Ave

Boston, MA 02215

Publications View

Inhibition of USP10 induces degradation of oncogenic FLT3.

Authors: Authors: Weisberg EL, Schauer NJ, Yang J, Lamberto I, Doherty L, Bhatt S, Nonami A, Meng C, Letai A, Wright R, Tiv H, Gokhale PC, Ritorto MS, De Cesare V, Trost M, Christodoulou A, Christie A, Weinstock DM, Adamia S, Stone R, Chauhan D, Anderson KC, Seo HS, Dhe-Paganon S, Sattler M, Gray NS, Griffin JD, Buhrlage SJ.
Nat Chem Biol 2017-12-01
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Characterization of midostaurin as a dual inhibitor of FLT3 and SYK and potentiation of FLT3 inhibition against FLT3-ITD-driven leukemia harboring activated SYK kinase.

Authors: Authors: Weisberg EL, Puissant A, Stone R, Sattler M, Buhrlage SJ, Yang J, Manley PW, Meng C, Buonopane M, Daley JF, Lazo S, Wright R, Weinstock DM, Christie AL, Stegmaier K, Griffin JD.
Oncotarget 2017-08-08
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Characterization of midostaurin as a dual inhibitor of FLT3 and SYK and potentiation of FLT3 inhibition against FLT3-ITD-driven leukemia harboring activated SYK kinase.

A brain-penetrant RAF dimer antagonist for the noncanonical BRAF oncoprotein of pediatric low-grade astrocytomas.

Authors: Authors: Sun Y, Alberta JA, Pilarz C, Calligaris D, Chadwick EJ, Ramkissoon SH, Ramkissoon LA, Garcia VM, Mazzola E, Goumnerova L, Kane M, Yao Z, Kieran MW, Ligon KL, Hahn WC, Garraway LA, Rosen N, Gray NS, Agar NY, Buhrlage SJ, Segal RA, Stiles CD.
Neuro Oncol 2017-06-01
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Targeting Myddosome Assembly in Waldenstrom Macroglobulinaemia.

Authors: Authors: Liu X, Hunter ZR, Xu L, Chen J, Chen JG, Tsakmaklis N, Patterson CJ, Castillo JJ, Buhrlage S, Gray N, Treon SP, Yang G.
Br J Haematol 2017-06-01
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Copy-number and gene dependency analysis reveals partial copy loss of wild-type SF3B1 as a novel cancer vulnerability.

Authors: Authors: Paolella BR, Gibson WJ, Urbanski LM, Alberta JA, Zack TI, Bandopadhayay P, Nichols CA, Agarwalla PK, Brown MS, Lamothe R, Yu Y, Choi PS, Obeng EA, Heckl D, Wei G, Wang B, Tsherniak A, Vazquez F, Weir BA, Root DE, Cowley GS, Buhrlage SJ, Stiles CD, Ebert BL, Hahn WC, Reed R, Beroukhim R.
Elife 2017-02-08
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Leveraging Gas-Phase Fragmentation Pathways for Improved Identification and Selective Detection of Targets Modified by Covalent Probes.

Authors: Authors: Ficarro SB, Browne CM, Card JD, Alexander WM, Zhang T, Park E, McNally R, Dhe-Paganon S, Seo HS, Lamberto I, Eck MJ, Buhrlage SJ, Gray NS, Marto JA.
Anal Chem 2016-12-20
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Pathophysiological significance and therapeutic targeting of germinal center kinase in diffuse large B-cell lymphoma.

Authors: Authors: Matthews JM, Bhatt S, Patricelli MP, Nomanbhoy TK, Jiang X, Natkunam Y, Gentles AJ, Martinez E, Zhu D, Chapman JR, Cortizas E, Shyam R, Chinichian S, Advani R, Tan L, Zhang J, Choi HG, Tibshirani R, Buhrlage SJ, Gratzinger D, Verdun R, Gray NS, Lossos IS.
Blood 2016-07-14
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HCK is a survival determinant transactivated by mutated MYD88, and a direct target of ibrutinib.

Authors: Authors: Yang G, Buhrlage SJ, Tan L, Liu X, Chen J, Xu L, Tsakmaklis N, Chen JG, Patterson CJ, Brown JR, Castillo JJ, Zhang W, Zhang X, Liu S, Cohen P, Hunter ZR, Gray N, Treon SP.
Blood 2016-06-23
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Inhibiting fungal multidrug resistance by disrupting an activator-Mediator interaction.

Authors: Authors: Nishikawa JL, Boeszoermenyi A, Vale-Silva LA, Torelli R, Posteraro B, Sohn YJ, Ji F, Gelev V, Sanglard D, Sanguinetti M, Sadreyev RI, Mukherjee G, Bhyravabhotla J, Buhrlage SJ, Gray NS, Wagner G, Näär AM, Arthanari H.
Nature 2016-02-25
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