TY - JOUR
T1 - Metalloallostery and Transition Metal Signaling
T2 - Bioinorganic Copper Chemistry Beyond Active Sites
AU - Pham, Vanha N.
AU - Chang, Christopher J.
N1 - Publisher Copyright:
© 2023 Wiley-VCH GmbH.
PY - 2023/3/6
Y1 - 2023/3/6
N2 - Transition metal chemistry is essential to life, where metal binding to DNA, RNA, and proteins underpins all facets of the central dogma of biology. In this context, metals in proteins are typically studied as static active site cofactors. However, the emergence of transition metal signaling, where mobile metal pools can transiently bind to biological targets beyond active sites, is expanding this conventional view of bioinorganic chemistry. This Minireview focuses on the concept of metalloallostery, using copper as a canonical example of how metals can regulate protein function by binding to remote allosteric sites (e.g., exosites). We summarize advances in and prospects for the field, including imaging dynamic transition metal signaling pools, allosteric inhibition or activation of protein targets by metal binding, and metal-dependent signaling pathways that underlie nutrient vulnerabilities in diseases spanning obesity, fatty liver disease, cancer, and neurodegeneration.
AB - Transition metal chemistry is essential to life, where metal binding to DNA, RNA, and proteins underpins all facets of the central dogma of biology. In this context, metals in proteins are typically studied as static active site cofactors. However, the emergence of transition metal signaling, where mobile metal pools can transiently bind to biological targets beyond active sites, is expanding this conventional view of bioinorganic chemistry. This Minireview focuses on the concept of metalloallostery, using copper as a canonical example of how metals can regulate protein function by binding to remote allosteric sites (e.g., exosites). We summarize advances in and prospects for the field, including imaging dynamic transition metal signaling pools, allosteric inhibition or activation of protein targets by metal binding, and metal-dependent signaling pathways that underlie nutrient vulnerabilities in diseases spanning obesity, fatty liver disease, cancer, and neurodegeneration.
KW - Copper Fluorescent Sensor
KW - Cuproplasia
KW - Cuproptosis
KW - Metalloallostery
KW - Transition Metal Signaling
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U2 - 10.1002/anie.202213644
DO - 10.1002/anie.202213644
M3 - Short survey
C2 - 36653724
AN - SCOPUS:85146482225
SN - 1433-7851
VL - 62
JO - Angewandte Chemie - International Edition
JF - Angewandte Chemie - International Edition
IS - 11
M1 - e202213644
ER -