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Literature DB >> 26957636

Combinatorial protein engineering of proteolytically resistant mesotrypsin inhibitors as candidates for cancer therapy.

Itay Cohen¹, Olumide Kayode², Alexandra Hockla², Banumathi Sankaran³, Derek C Radisky², Evette S Radisky⁴, Niv Papo⁵.

Abstract

Engineered protein therapeutics offer advantages, including strong target affinity, selectivity and low toxicity, but like natural proteins can be susceptible to proteolytic degradation, thereby limiting their effectiveness. A compelling therapeutic target is mesotrypsin, a protease up-regulated with tumour progression, associated with poor prognosis, and implicated in tumour growth and progression of many cancers. However, with its unique capability for cleavage and inactivation of proteinaceous inhibitors, mesotrypsin presents a formidable challenge to the development of biological inhibitors. We used a powerful yeast display platform for directed evolution, employing a novel multi-modal library screening strategy, to engineer the human amyloid precursor protein Kunitz protease inhibitor domain (APPI) simultaneously for increased proteolytic stability, stronger binding affinity and improved selectivity for mesotrypsin inhibition. We identified a triple mutant APPIM17G/I18F/F34V, with a mesotrypsin inhibition constant (Ki) of 89 pM, as the strongest mesotrypsin inhibitor yet reported; this variant displays 1459-fold improved affinity, up to 350 000-fold greater specificity and 83-fold improved proteolytic stability compared with wild-type APPI. We demonstrated that APPIM17G/I18F/F34V acts as a functional inhibitor in cell-based models of mesotrypsin-dependent prostate cancer cellular invasiveness. Additionally, by solving the crystal structure of the APPIM17G/I18F/F34V-mesotrypsin complex, we obtained new insights into the structural and mechanistic basis for improved binding and proteolytic resistance. Our study identifies a promising mesotrypsin inhibitor as a starting point for development of anticancer protein therapeutics and establishes proof-of-principle for a novel library screening approach that will be widely applicable for simultaneously evolving proteolytic stability in tandem with desired functionality for diverse protein scaffolds.

Entities: CellLine Chemical Disease Gene Mutation Species

Keywords: X-ray structure; cancer therapy; directed evolution; enzyme inhibition; mesotrypsin; protease inhibitor; protein engineering; proteolysis

Mesh：

Substances：

Year: 2016 PMID： 26957636 PMCID： PMC4898653 DOI： 10.1042/BJ20151410

Source DB: PubMed Journal: Biochem J ISSN： 0264-6021 Impact factor: 3.857

56 in total

1. Directed evolution of a stable scaffold for T-cell receptor engineering.

Authors: E V Shusta; P D Holler; M C Kieke; D M Kranz; K D Wittrup
Journal: Nat Biotechnol Date: 2000-07 Impact factor: 54.908

2. Directed evolution of a protein: selection of potent neutrophil elastase inhibitors displayed on M13 fusion phage.

Authors: B L Roberts; W Markland; A C Ley; R B Kent; D W White; S K Guterman; R C Ladner
Journal: Proc Natl Acad Sci U S A Date: 1992-03-15 Impact factor: 11.205

3. Cloning, characterization and nucleotide sequences of two cDNAs encoding human pancreatic trypsinogens.

Authors: M Emi; Y Nakamura; M Ogawa; T Yamamoto; T Nishide; T Mori; K Matsubara
Journal: Gene Date: 1986 Impact factor: 3.688

4. Crystal structure reveals basis for the inhibitor resistance of human brain trypsin.

Authors: Gergely Katona; Gunnar I Berglund; Janos Hajdu; László Gráf; László Szilágyi
Journal: J Mol Biol Date: 2002-02-01 Impact factor: 5.469

5. Presence versus absence of hydrogen bond donor Tyr-39 influences interactions of cationic trypsin and mesotrypsin with protein protease inhibitors.

Authors: Moh'd A Salameh; Alexei S Soares; Alexandre Alloy; Evette S Radisky
Journal: Protein Sci Date: 2012-06-25 Impact factor: 6.725

6. Engineering kunitz domain 1 (KD1) of human tissue factor pathway inhibitor-2 to selectively inhibit fibrinolysis: properties of KD1-L17R variant.

Authors: Madhu S Bajaj; Godwin I Ogueli; Yogesh Kumar; Kanagasabai Vadivel; Gregory Lawson; Sreejesh Shanker; Amy E Schmidt; S Paul Bajaj
Journal: J Biol Chem Date: 2010-11-29 Impact factor: 5.157

7. Iterative optimization of high-affinity protease inhibitors using phage display. 2. Plasma kallikrein and thrombin.

Authors: W Markland; A C Ley; R C Ladner
Journal: Biochemistry Date: 1996-06-18 Impact factor: 3.162

8. Directed evolution of the epidermal growth factor receptor extracellular domain for expression in yeast.

Authors: Yong-Sung Kim; Rashna Bhandari; Jennifer R Cochran; John Kuriyan; K Dane Wittrup
Journal: Proteins Date: 2006-03-01

9. S100 family members and trypsinogens are predictors of distant metastasis and survival in early-stage non-small cell lung cancer.

Authors: Sven Diederichs; Etmar Bulk; Björn Steffen; Ping Ji; Lara Tickenbrock; Kerstin Lang; Kurt S Zänker; Ralf Metzger; Paul M Schneider; Volker Gerke; Michael Thomas; Wolfgang E Berdel; Hubert Serve; Carsten Müller-Tidow
Journal: Cancer Res Date: 2004-08-15 Impact factor: 12.701

10. Mesotrypsin promotes malignant growth of breast cancer cells through shedding of CD109.

Authors: Alexandra Hockla; Derek C Radisky; Evette S Radisky
Journal: Breast Cancer Res Treat Date: 2009-12-25 Impact factor: 4.872

17 in total

1. An Acrobatic Substrate Metamorphosis Reveals a Requirement for Substrate Conformational Dynamics in Trypsin Proteolysis.

Authors: Olumide Kayode; Ruiying Wang; Devon F Pendlebury; Itay Cohen; Rachel D Henin; Alexandra Hockla; Alexei S Soares; Niv Papo; Thomas R Caulfield; Evette S Radisky
Journal: J Biol Chem Date: 2016-11-03 Impact factor: 5.157

Review 2. Tailoring Proteins to Re-Evolve Nature: A Short Review.

Authors: Angelica Jimenez-Rosales; Miriam V Flores-Merino
Journal: Mol Biotechnol Date: 2018-12 Impact factor: 2.695

3. Pre-equilibrium competitive library screening for tuning inhibitor association rate and specificity toward serine proteases.

Authors: Itay Cohen; Si Naftaly; Efrat Ben-Zeev; Alexandra Hockla; Evette S Radisky; Niv Papo
Journal: Biochem J Date: 2018-04-16 Impact factor: 3.857

4. Disulfide engineering of human Kunitz-type serine protease inhibitors enhances proteolytic stability and target affinity toward mesotrypsin.

Authors: Itay Cohen; Matt Coban; Anat Shahar; Banumathi Sankaran; Alexandra Hockla; Shiran Lacham; Thomas R Caulfield; Evette S Radisky; Niv Papo
Journal: J Biol Chem Date: 2019-01-30 Impact factor: 5.157

5. A Camelid-derived Antibody Fragment Targeting the Active Site of a Serine Protease Balances between Inhibitor and Substrate Behavior.

Authors: Tobias Kromann-Hansen; Emil Oldenburg; Kristen Wing Yu Yung; Gholamreza H Ghassabeh; Serge Muyldermans; Paul J Declerck; Mingdong Huang; Peter A Andreasen; Jacky Chi Ki Ngo
Journal: J Biol Chem Date: 2016-05-23 Impact factor: 5.157

6. A computational combinatorial approach identifies a protein inhibitor of superoxide dismutase 1 misfolding, aggregation, and cytotoxicity.

Authors: Victor Banerjee; Ofek Oren; Efrat Ben-Zeev; Ran Taube; Stanislav Engel; Niv Papo
Journal: J Biol Chem Date: 2017-08-02 Impact factor: 5.157

7. A potent, proteolysis-resistant inhibitor of kallikrein-related peptidase 6 (KLK6) for cancer therapy, developed by combinatorial engineering.

Authors: Amiram Sananes; Itay Cohen; Anat Shahar; Alexandra Hockla; Elena De Vita; Aubry K Miller; Evette S Radisky; Niv Papo
Journal: J Biol Chem Date: 2018-06-22 Impact factor: 5.157