Scalable synthesis and structural characterization of reversible KLK6 inhibitors

Andreas Baumann; Daniel Isak; Jasmin Lohbeck; Pravin Kumar Ankush Jagtap; Janosch Hennig; Aubry K. Miller

doi:10.1039/d2ra04670a

Scalable synthesis and structural characterization of reversible KLK6 inhibitors

Andreas Baumann
, Daniel Isak
, Jasmin Lohbeck
, Pravin Kumar Ankush Jagtap
, Janosch Hennig
, Aubry K. Miller^*

^*Corresponding author for this work

Biosciences

Research output: Contribution to journal › Article › peer-review

Abstract

Scalable asymmetric syntheses of two kallikrein-related protease 6 (KLK6) inhibitors are reported. The inhibitors are assembled by linking enantiomerically enriched fragments via amide bond formation, followed by conversion of a cyano group to an amidine. One fragment, an amine, was prepared using the Ellman auxiliary, and a lack of clarity in the literature regarding the stereochemical outcome of this reaction was solved via X-ray crystallographic analysis of two derivatives. Complexes of the inhibitors bound to human KLK6 were solved by X-ray crystallography, revealing the binding poses.

Original language	English
Pages (from-to)	26989-26993
Number of pages	5
Journal	RSC Advances
Volume	12
Issue number	41
DOIs	https://doi.org/10.1039/d2ra04670a
Publication status	Published - 21 Sept 2022

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This journal is © The Royal Society of Chemistry.

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title = "Scalable synthesis and structural characterization of reversible KLK6 inhibitors",

abstract = "Scalable asymmetric syntheses of two kallikrein-related protease 6 (KLK6) inhibitors are reported. The inhibitors are assembled by linking enantiomerically enriched fragments via amide bond formation, followed by conversion of a cyano group to an amidine. One fragment, an amine, was prepared using the Ellman auxiliary, and a lack of clarity in the literature regarding the stereochemical outcome of this reaction was solved via X-ray crystallographic analysis of two derivatives. Complexes of the inhibitors bound to human KLK6 were solved by X-ray crystallography, revealing the binding poses.",

author = "Andreas Baumann and Daniel Isak and Jasmin Lohbeck and Jagtap, \{Pravin Kumar Ankush\} and Janosch Hennig and Miller, \{Aubry K.\}",

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AU - Baumann, Andreas

AU - Isak, Daniel

AU - Lohbeck, Jasmin

AU - Jagtap, Pravin Kumar Ankush

AU - Hennig, Janosch

AU - Miller, Aubry K.

PY - 2022/9/21

Y1 - 2022/9/21

N2 - Scalable asymmetric syntheses of two kallikrein-related protease 6 (KLK6) inhibitors are reported. The inhibitors are assembled by linking enantiomerically enriched fragments via amide bond formation, followed by conversion of a cyano group to an amidine. One fragment, an amine, was prepared using the Ellman auxiliary, and a lack of clarity in the literature regarding the stereochemical outcome of this reaction was solved via X-ray crystallographic analysis of two derivatives. Complexes of the inhibitors bound to human KLK6 were solved by X-ray crystallography, revealing the binding poses.

AB - Scalable asymmetric syntheses of two kallikrein-related protease 6 (KLK6) inhibitors are reported. The inhibitors are assembled by linking enantiomerically enriched fragments via amide bond formation, followed by conversion of a cyano group to an amidine. One fragment, an amine, was prepared using the Ellman auxiliary, and a lack of clarity in the literature regarding the stereochemical outcome of this reaction was solved via X-ray crystallographic analysis of two derivatives. Complexes of the inhibitors bound to human KLK6 were solved by X-ray crystallography, revealing the binding poses.

U2 - 10.1039/d2ra04670a

DO - 10.1039/d2ra04670a

M3 - Article

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SP - 26989

EP - 26993

JO - RSC Advances

JF - RSC Advances

IS - 41

ER -

Scalable synthesis and structural characterization of reversible KLK6 inhibitors

Abstract

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