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Author Correction: Selective inhibitors of JAK1 targeting an isoform-restricted allosteric cysteine

Madeline E. Kavanagh
Benjamin D. Horning
Benjamin F. Cravatt
Amendments and Corrections30 Sept 2022
Nature Chemical Biology

Volume: 18, P: 1288
Altered Hox expression and segmental identity in Mll-mutant mice

Benjamin D. Yu
Jay L. Hess
Stanley J. Korsmeyer
Research30 Nov 1995
Nature

Volume: 378, P: 505-508
Selective inhibitors of JAK1 targeting an isoform-restricted allosteric cysteine

Chemical proteomics identified covalent ligands targeting an isoform-restricted allosteric cysteine in JAK1. The compounds inhibit JAK1-dependent signaling in immune cells with unprecedented selectivity.

Madeline E. Kavanagh
Benjamin D. Horning
Benjamin F. Cravatt
Research12 Sept 2022
Nature Chemical Biology

Volume: 18, P: 1388-1398
Chemoproteomic profiling and discovery of protein electrophiles in human cells

A chemical proteomic strategy is described for the discovery of protein-bound electrophilic groups in human cells. Using this approach, the dynamic regulation of the pyruvoyl catalytic cofactor in S-adenosyl-L-methionine decarboxylase was characterized and an N-terminal glyoxylyl modification on secernin proteins was discovered.

Megan L. Matthews
Lin He
Benjamin F. Cravatt
Research31 Oct 2016
Nature Chemistry

Volume: 9, P: 234-243
Proteome-wide covalent ligand discovery in native biological systems

Small molecules are powerful tools for investigating protein function, and can serve as leads for new therapeutics, but most human proteins lack known small-molecule ligands; here, a quantitative analysis of cysteine-reactive small-molecule fragments screened against thousands of proteins is reported.

Keriann M. Backus
Bruno E. Correia
Benjamin F. Cravatt
Research15 Jun 2016
Nature

Volume: 534, P: 570-574
High-level semi-synthetic production of the potent antimalarial artemisinin

Saccharomyces cerevisiae is engineered to produce high concentrations of artemisinic acid, a precursor of the artemisinin used in combination therapies for malaria treatment; an efficient and practical chemical process to convert artemisinic acid to artemisinin is also developed.

C. J. Paddon
P. J. Westfall
J. D. Newman
Research10 Apr 2013
Nature

Volume: 496, P: 528-532
Cellular and molecular signal transduction pathways modulated by rituximab (rituxan, anti-CD20 mAb) in non-Hodgkin's lymphoma: implications in chemosensitization and therapeutic intervention

Ali R Jazirehi
Benjamin Bonavida
Reviews24 Mar 2005
Oncogene

Volume: 24, P: 2121-2143
Rewriting yeast central carbon metabolism for industrial isoprenoid production

Yeast central carbon metabolism has been engineered to achieve a more efficient isoprenoid biosynthesis pathway, an advance that brings commodity-scale production of such compounds a step closer.

Adam L. Meadows
Kristy M. Hawkins
Annie E. Tsong
Research21 Sept 2016
Nature

Volume: 537, P: 694-697

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Author Correction: Selective inhibitors of JAK1 targeting an isoform-restricted allosteric cysteine

Altered Hox expression and segmental identity in Mll-mutant mice

Selective inhibitors of JAK1 targeting an isoform-restricted allosteric cysteine

Chemoproteomic profiling and discovery of protein electrophiles in human cells

Proteome-wide covalent ligand discovery in native biological systems

High-level semi-synthetic production of the potent antimalarial artemisinin

Cellular and molecular signal transduction pathways modulated by rituximab (rituxan, anti-CD20 mAb) in non-Hodgkin's lymphoma: implications in chemosensitization and therapeutic intervention

Rewriting yeast central carbon metabolism for industrial isoprenoid production

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