Author: Orba, Yasuko ; Sato, Akihiko ; Sawa, Hirofumi ; Sasaki, Michihito ; Maruyama, Yuki ; Hall, William W ; Miki, Shigeru ; Sanaki, Takao ; Kusakabe, Shinji ; Toba, Shinsuke ; Uemura, Kentaro ; Iimuro, Atsuhiro ; Shishido, Takao ; Konishi, Kei

The spike (S) protein of Severe Acute Respiratory Syndrome Coronavirus-2 (SARS-CoV-2) binds to a host cell receptor which dictates the viral entry pathway. SARS-CoV-2 utilizes two different pathways for cellular entry mediated by both a host type II transmembrane serine protease (TMPRSS2) and cathepsin proteases. These host proteases cleave the viral S protein and initiate membrane fusion allowing viral infection. We previously isolated a SARS-CoV-2 mutant with deletion in the furin cleavage site of the S gene (del2) and revealed differences in cell tropism between wild-type (WT) and del2 viruses. Here, we evaluated the antiviral activities of cellular protease inhibitors against SARS-CoV-2 WT and del2 viruses using several different cell lines. The TMPRSS2 inhibitor, camostat, exhibited strong antiviral activity against WT virus but not del2, while the cathepsin B/L inhibitor, K11777, exhibited potent antiviral activity against the del2 virus. We isolated K11777-escape mutants of SARS-CoV-2 and SARS-CoV and demonstrated that these mutations facilitated S protein cleavage at the S2' site mediated by cathepsin L. Finally, we demonstrated that combination treatment of K11777 and camostat potently inhibited SARS-CoV-2 WT infection in vitro and in vivo, suggesting the usefulness of combination therapeutics targeting host TMPRSS2 and cathepsin proteases against coronavirus infection. In summary, our study characterized K11777 as an inhibitor of S2' cleavage by cathepsins, highlighting the critical role of the S2' site in SARS-CoV-2 cellular entry. This research sheds light on the infection process and has implications for potential therapeutic interventions for SARS-CoV-2 infection.

09 Jan 2025·ACS Medicinal Chemistry Letters

Discovery of a Potent Triazole-Based Reversible Targeted Covalent Inhibitor of Cruzipain

Article

Author: Quevedo, Mario Alfredo ; Cerutti, Juan Pablo ; Dehaen, Wim ; Diniz, Lucas Abreu ; Vilchez Larrea, Salomé Catalina ; Alonso, Guillermo Daniel ; Corrêa Santos, Viviane ; Ferreira, Rafaela Salgado

Cruzipain (CZP) is an essential cysteine protease of Trypanosoma cruzi, the etiological agent of Chagas disease, and a promising druggable target. To date, no CZP inhibitors have reached clinical use, with research efforts mostly hampered by insufficient potency, limited target selectivity or lack of bioactivity translation from the isolated enzyme to the parasite in cellular environments. In this study, we report the design of SH-1, a 1,2,3-triazole-based targeted covalent inhibitor with nanomolar potency (IC₅₀ = 28 nM) and null inhibition of human cathepsin L. SH-1 demonstrates bioactivity translation comparable to that of K777 (1-10 μM), a CZP inhibitor previously advanced to clinical trials. Experimental findings indicate that SH-1 forms a reversible covalent bond with Cys25 in CZP, while in silico and structure-activity relationship studies suggest that this interaction is guided by acid-base equilibrium dynamics. The potential of SH-1 for preclinical development is discussed alongside detailed structure-activity relationships for the further optimization of CZP inhibitors.

01 Dec 2024·BIOORGANIC CHEMISTRY

Rhodesain inhibitors on the edge of reversibility-irreversibility

Article

Author: González, Florenci V. ; Agost-Beltrán, Laura ; Räder, Hans Joachim ; Schirmeister, Tanja ; Kersten, Christian ; González, Florenci V ; Rodríguez, Santiago ; Zimmer, Collin

A comparative study of Michael acceptor and keto-Michael acceptor inhibitors of the cysteine protease rhodesain has been performed. Five new inhibitors have been prepared bearing the peptide structure of the known cysteine protease inhibitor K11777 and differing on the warhead. For the preparation of the Michael acceptor warhead, a Horner-Wadsworth-Emmons reaction was used. In the synthetic routes of the keto-Michael acceptor warheads, keto-enoate and keto-vinyl sulfone, a metathesis reaction and a radical sulfonylation were the key steps, respectively. Interestingly, keto-Michael acceptors inhibited rhodesain through a dual mode of action, showing reversibility at low inhibitor concentrations and irreversibility at high inhibitor concentrations.

News (Medical) associated with K-777

15 May 2024

·www.sciencedaily.com

An active agent against hepatitis E

At present, there is no specific active substance against hepatitis E. As the disease kills 70,000 people every year, researchers are actively searching for one. A team may have found what they're looking for. The researchers showed that the compound K11777 prevents host cells from helping the virus out of its shell by cleaving the viral capsid. This means it can no longer infect cells. At present, there is no specific active substance against hepatitis E. As the disease kills 70,000 people every year, researchers are actively searching for one. The team from the Department of Molecular and Medical Virology at Ruhr University Bochum, Germany, may have found what they're looking for. The researchers showed that the compound K11777 prevents host cells from helping the virus out of its shell by cleaving the viral capsid. This means it can no longer infect cells. "The compound is already being tested in clinical trials against other viruses such as Sars-Cov-2," says lead author Mara Klöhn. "There's still a lot of work to be done to find out whether it can be used as an active substance against hepatitis E, but it's a first step." The researchers published their findings on May, 11, 2024 in the journal Hepatology. In order to infect an organ, viruses need the help of the host cells. "An effective approach is therefore to identify targets in the host that can be manipulated by drugs so that they no longer perform this helper function," explains Mara Klöhn. The researchers became aware of the compound K11777 in a roundabout way: During a control study conducted as part of cell culture studies on the hepatitis C virus with a known active ingredient, they discovered that this active ingredient was also effective against hepatitis E. "However, the drug wasn't using the same pathway as with the hepatitis C virus, because the hepatitis E virus doesn't have the target structure that this active substance attacks," explains Mara Klöhn. This suggested that the drug may have an effect on host cells instead. The research team narrowed down the possible target structures and turned their attention to cathepsins, which can process proteins, i.e. cleave them. K11777 inhibits many cathepsin types, i.e. blocks their function. Tests in cell culture with human liver cells showed that the compound actually prevents infection with hepatitis E viruses. "In follow-up experiments, we proved our hypothesis that the compound prevents cathepsin L from cleaving and opening up the viral capsid," says Mara Klöhn. "This means that the virus can no longer infect host cells." Hepatitis E The hepatitis E virus (HEV) is the main cause of acute viral hepatitis. Approximately 70,000 people die from the disease every year. After the first documented epidemic outbreak between 1955 and 1956, more than 50 years passed before researchers began to address the issue in depth. Acute infections usually clear up spontaneously in patients with an intact immune system. In patients with a reduced or suppressed immune system, such as organ transplant recipients or people infected with HIV, HEV can become chronic. HEV also poses a serious threat to pregnant women. There aren't any vaccines nor specific active substances against the virus.

100 Deals associated with K-777

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Indication	Highest Phase	Country/Location	Organization	Date
Chagas Disease	Preclinical	United States	Cornell University	01 Dec 2005

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