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Proteases—From Basic Structure to Function to Drug Design as Targeted Therapy



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Autore: Kwok Hang Fai Visualizza persona
Titolo: Proteases—From Basic Structure to Function to Drug Design as Targeted Therapy Visualizza cluster
Pubblicazione: Basel, Switzerland, : MDPI - Multidisciplinary Digital Publishing Institute, 2021
Descrizione fisica: 1 electronic resource (93 p.)
Soggetto topico: Research & information: general
Soggetto non controllato: MMP
MMP2
MMP9
MMP7
MMP14
matrix metalloproteases
PDAC
pancreatic cancer
Bowman–Birk inhibitor
ranacyclin
trypsin inhibitor
structure–activity relationship
synergistic effect
Gentamicin
matrix metalloproteinase
extracellular matrix
nuclei
cancer
apoptosis
immune response
cysteine protease inhibitor
stefin
signal peptide
parasite
phylogenetic analysis
diversification
protein structure
vascular endothelial growth factors (VEGFs)
VEGF-A
PlGF
VEGF-B
VEGF-C
VEGF-D
angiogenesis
lymphangiogenesis
CCBE1
proteases
ADAMTS3
plasmin
cathepsin D
KLK3
prostate-specific antigen (PSA)
thrombin
wound healing
metastasis
proteolytic activation
vascular biology
lymphedema
Persona (resp. second.): ShawChristopher
WalkerBrian
KwokHang Fai
Sommario/riassunto: In the two last decades, proteases have constituted one of the primary and important targets in drug discovery. The U.S. FDA has approved more than 12 protease therapies in the last 10 years, and a number of next-generation or completely new proteases are under clinical development. Protease inhibition strategies are one of the fastest expanding areas in the field of of drugs that show considerable promise. This Special Issue will focus on the recent advances in the discovery and development of protease inhibitors, covering the synthesis of protease inhibitors, the design of new chemical entities acting as inhibitors of special/particular types of proteases, and their mode of actions (Frolova et al. 2020; Slapak et al. 2020; Künnapuu et al. 2021). In addition, the new applications of these interesting compounds/biomolecules and their limitations have been discussed and described (Wang et al. 2020; Bartošová-Sojková et al. 2021).
Titolo autorizzato: Proteases—From Basic Structure to Function to Drug Design as Targeted Therapy  Visualizza cluster
Formato: Materiale a stampa
Livello bibliografico Monografia
Lingua di pubblicazione: Inglese
Record Nr.: 9910557353103321
Lo trovi qui: Univ. Federico II
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