Bioorthogonal chemistry

被引:0
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作者
Samuel L. Scinto
Didier A. Bilodeau
Robert Hincapie
Wankyu Lee
Sean S. Nguyen
Minghao Xu
Christopher W. am Ende
M. G. Finn
Kathrin Lang
Qing Lin
John Paul Pezacki
Jennifer A. Prescher
Marc S. Robillard
Joseph M. Fox
机构
[1] University of Delaware,Department of Chemistry and Biochemistry
[2] University of Ottawa,Department of Chemistry and Biomolecular Science
[3] Georgia Institute of Technology,School of Chemistry and Biochemistry
[4] Pfizer Worldwide Research and Development,Department of Chemistry
[5] University of California,Department of Chemistry
[6] Pfizer Worldwide Research and Development,Department of Chemistry
[7] Technical University of Munich,Molecular Biology & Biochemistry
[8] Laboratory of Organic Chemistry,undefined
[9] State University of New York at Buffalo,undefined
[10] University of California,undefined
[11] Tagworks Pharmaceuticals,undefined
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摘要
Bioorthogonal chemistry represents a class of high-yielding chemical reactions that proceed rapidly and selectively in biological environments without side reactions towards endogenous functional groups. Rooted in the principles of physical organic chemistry, bioorthogonal reactions are intrinsically selective transformations not commonly found in biology. Key reactions include native chemical ligation and the Staudinger ligation, copper-catalysed azide–alkyne cycloaddition, strain-promoted [3 + 2] reactions, tetrazine ligation, metal-catalysed coupling reactions, oxime and hydrazone ligations as well as photoinducible bioorthogonal reactions. Bioorthogonal chemistry has significant overlap with the broader field of ‘click chemistry’ — high-yielding reactions that are wide in scope and simple to perform, as recently exemplified by sulfuryl fluoride exchange chemistry. The underlying mechanisms of these transformations and their optimal conditions are described in this Primer, followed by discussion of how bioorthogonal chemistry has become essential to the fields of biomedical imaging, medicinal chemistry, protein synthesis, polymer science, materials science and surface science. The applications of bioorthogonal chemistry are diverse and include genetic code expansion and metabolic engineering, drug target identification, antibody–drug conjugation and drug delivery. This Primer describes standards for reproducibility and data deposition, outlines how current limitations are driving new research directions and discusses new opportunities for applying bioorthogonal chemistry to emerging problems in biology and biomedicine.
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