Selective Nonpeptidic Inhibitors of Herpes Simplex Virus Type 1 and Human Cytomegalovirus Proteases.

Matsumoto, Mitsuhiro; Misawa, S.; Chiba, Nobuyoshi; Takaku, Haruo; Hayashi, Hideya

doi:10.1248/bpb.24.236

Cited by 11 publications

(2 citation statements)

References 32 publications

(26 reference statements)

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“…Несмотря на сходство структур, 1,4-дигидроксинафталин ингибирует протеазу ВПГ-1 по конкурентному механизму, тогда как 3 нафтохинона являются неконкурентными ингибиторами. Действие этих соединений селективно в отношении герпетических протеаз, они не проявляют существенной ингибирующей активности против сериновых протеаз млекопитающих (химотрипсин, трипсин, калликреин, плазмин, тромбин и фактор Xa) в концентрации 100 мкМ [43]. Таким образом, вышеописанные непептидные соединения могут представлять интерес для дальнейшего изучения их активности in vivo.…”

Section: ингибиторы герпетической протеазыunclassified

Modern Ethiotropic Chemotherapy of Herpesvirus Infections: Advances, New Trends and Perspectives. Alphaherpesviruses (Part Ii)

Андронова¹

2018

Problems of Virology

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A key role in the treatment of herpesviral infections is played by modified nucleosides and their predecessors - acyclovir, its L-valine ester (valaciclovir) and famciclovir (prodrug of penciclovir). The biological activity of compounds of this class is determined by their similarity to natural nucleosides. After phosphorylation by viral thymidine kinase and then cell enzymes to the triphosphate forms, acyclovir and penciclovir inhibit the activity of viral DNA polymerase and synthesis of viral DNA. The increasing role of herpesvirus infections in human infectious pathology, as well as the development of drug resistance in viruses, mainly in patients with immunodeficiencies of various origins, necessitate the search for new compounds possessing anti-herpesvirus activity, using as a biological target not DNA polymerase, but other viral proteins and enzymes, unique or different from cellular proteins, performing similar functions.

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Section: ингибиторы герпетической протеазыunclassified

Modern Ethiotropic Chemotherapy of Herpesvirus Infections: Advances, New Trends and Perspectives. Alphaherpesviruses (Part Ii)

Андронова¹

2018

Problems of Virology

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“…Through screening of a compound library, Matsumoto et al (2001) discovered 4 compounds, 1,4-dihydroxynaphthalene and 3 naphthoquinones, which effectively inhibit HSV-1 protease. Further study indicated that these compounds were potent and selective inhibitors of CMV protease, with extremely low IC 50 values.…”

Section: Herpes Virusesmentioning

confidence: 99%

Protease inhibitors and their peptidomimetic derivatives as potential drugs

Fear

Komarnytsky

Raskin

2007

Pharmacology & Therapeutics

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Precise spatial and temporal regulation of proteolytic activity is essential to human physiology. Modulation of protease activity with synthetic peptidomimetic inhibitors has proven to be clinically useful for treating human immunodeficiency virus (HIV) and hypertension and shows potential for medicinal application in cancer, obesity, cardiovascular, inflammatory, neurodegenerative diseases, and various infectious and parasitic diseases. Exploration of natural inhibitors and synthesis of peptidomimetic molecules has provided many promising compounds performing successfully in animal studies. Several protease inhibitors are undergoing further evaluation in human clinical trials. New research strategies are now focusing on the need for improved comprehension of protease-regulated cascades, along with precise selection of targets and improved inhibitor specificity. It remains to be seen which second generation agents will evolve into approved drugs or complementary therapies.

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Antiviral Agents, DNA

Middleton

Rockway

2003

Burger's Medicinal Chemistry and Drug Discovery

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The seven families of DNA viruses that cause disease in humans show tremendous variety in the relationships that they have with their hosts. This variety is reflected both in the disease states that they cause and the approaches used to develop antiviral drugs to treat them. The most successful antiviral tools have been nucleoside analogs, particularly those targeting the polymerases of herpesviruses and hepatitis virus B. The list of nucleoside analog drugs continues to expand as compounds are developed with greater potency or range, better bioavailability, or improved side effect profiles. Other viral targets have started to receive more attention, including helicases, proteases, and enzymes required for virion assembly. These targets should gain in importance as resistance to currently available drugs becomes more prevalent. In addition, expanding the list of viable viral targets is particularly important with regard to members of the parvovirus, papillomavirus, and polyomavirus families, which do not encode a viral polymerase. Some effective antiviral treatments have not targeted the virus but rather the immune response to the viral infection. An optimal immune response is critical to elimination of some classes of viruses, and exploiting this aspect of the host‐virus interaction provides another approach to antiviral drug development.

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Selective Nonpeptidic Inhibitors of Herpes Simplex Virus Type 1 and Human Cytomegalovirus Proteases.

Cited by 11 publications

References 32 publications

Modern Ethiotropic Chemotherapy of Herpesvirus Infections: Advances, New Trends and Perspectives. Alphaherpesviruses (Part Ii)

Modern Ethiotropic Chemotherapy of Herpesvirus Infections: Advances, New Trends and Perspectives. Alphaherpesviruses (Part Ii)

Protease inhibitors and their peptidomimetic derivatives as potential drugs

Antiviral Agents, DNA

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