Not all pycnodysostosis-related mutants of human cathepsin K are inactive - crystal structure and biochemical studies of an active mutant I249T

Sumana Roy; Sudeshna Das Chakraborty; Sampa Biswas

doi:10.1111/febs.14655

Not all pycnodysostosis-related mutants of human cathepsin K are inactive - crystal structure and biochemical studies of an active mutant I249T

FEBS J. 2018 Nov;285(22):4265-4280. doi: 10.1111/febs.14655. Epub 2018 Sep 26.

Authors

Sumana Roy¹, Sudeshna Das Chakraborty², Sampa Biswas^{1

3}

Affiliations

¹ Crystallography and Molecular Biology Division, Saha Institute of Nuclear Physics, Kolkata, India.
² Chemical Sciences Division, Saha Institute of Nuclear Physics, Kolkata, India.
³ Homi Bhaba National Institute, Mumbai, India.

PMID: 30199612
DOI: 10.1111/febs.14655

Abstract

Human cathepsin K (CTSK) is a collagenolytic lysosomal cysteine protease that plays an important role in bone turnover. Mutation in CTSK gene is associated with loss of collagenolytic activity of CTSK leading to an autosomal recessive bone disorder called pycnodysostosis. Although a number of pycnodysostotic missense mutations have been reported, underlying mechanism of the disease is not clear. In this study, we investigated in vitro six recombinant pycnodysostosis-related mutants of human CTSK (G79E, I249T, G243E, G303E, G319C and Q187P). While all the mutants, like wild-type, show similar high levels of expression in Escherichia coli, four of them (G79E, G303E, G319C and Q187P) are inactive, unstable and spontaneously degrade during purification process. In contrast, proteolytic/collagenolytic activity, zymogen activation kinetics and stability of G243E and I249T mutants are nominally affected. Crystal structure of I249T at 1.92 Å resolution shows that the mutation in R-domain causes conformational changes of a surface loop in the L-domain although the catalytic cleft remains unaltered. Molecular simulation, normal mode analysis and fluorescence lifetime measurement eliminated the possibility that the change in L-domain surface loop orientation is a crystallization artefact. CD-based thermal melting profile indicates that stability of I249T is significantly higher than wild-type. Our studies first time reports that pycnodysostosis-related mutations do not always lead to complete loss of general proteolytic activity or specific collagenolytic activity of CTSK. The first crystal structure of a pycnodysostotic mutant (I249T) provides critical information that may pave new avenues towards understanding the disease at molecular level. DATABASE: The atomic co-ordinates and structure factors for I249T mutant of human CTSK (codes 5Z5O) have been deposited in the Protein Data Bank (http://wwpdb.org/).

Keywords: X-ray structure; cathepsin K; collagenase; cysteine protease; pycnodysostosis.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Amino Acid Sequence
Catalysis
Cathepsin K / chemistry*
Cathepsin K / genetics
Cathepsin K / metabolism*
Crystallography, X-Ray
DNA Mutational Analysis
Humans
Models, Molecular
Mutation*
Protein Conformation
Pycnodysostosis / genetics*
Sequence Homology

Substances

CTSK protein, human
Cathepsin K