Anti-HIV-1 Activity of pepRF1, a Proteolysis-Resistant CXCR4 Antagonist Derived from Dengue Virus Capsid Protein

Iris Cadima-Couto; Alexandra Tauzin; Joaõ M. Freire; Tiago N. Figueira; Rúben D.M. Silva; Clara Pérez-Peinado; Catarina Cunha-Santos; Inês Bártolo; Nuno Taveira; Lurdes Gano; Joaõ D.G. Correia; Joao Goncalves; Fabrizio Mammano; David Andreu; Miguel A.R.B. Castanho; Ana Salomé Veiga

doi:10.1021/acsinfecdis.9b00507

Anti-HIV-1 Activity of pepRF1, a Proteolysis-Resistant CXCR4 Antagonist Derived from Dengue Virus Capsid Protein

Iris Cadima-Couto
, Alexandra Tauzin
, Joaõ M. Freire
, Tiago N. Figueira
, Rúben D.M. Silva
, Clara Pérez-Peinado
, Catarina Cunha-Santos
, Inês Bártolo
, Nuno Taveira
, Lurdes Gano
, Joaõ D.G. Correia
, Joao Goncalves
, Fabrizio Mammano
, David Andreu
, Miguel A.R.B. Castanho
, Ana Salomé Veiga

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4 Citações (Scopus)

Resumo

There is an urgent need for the development of new anti-HIV drugs that can complement existing medicines to be used against resistant strains. Here, we report the anti-HIV-1 peptide pepRF1, a human serum-resistant peptide derived from the Dengue virus capsid protein. In vitro, pepRF1 shows a 50% inhibitory concentration of 1.5 nM with a potential therapeutic window higher than 53â000. This peptide is specific for CXCR4-tropic strains, preventing viral entry into target cells by binding to the viral coreceptor CXCR4, acting as an antagonist of this receptor. pepRF1 is more effective than T20, the only peptide-based HIV-1 entry inhibitor approved, and excels in inhibiting a HIV-1 strain resistant to T20. Potentially, pepRF1 can be used alone or in combination with other anti-HIV drugs. Furthermore, one can also envisage its use as a novel therapeutic strategy for other CXCR4-related diseases.

Idioma original	???core.languages.en_GB???
Páginas (de-até)	6-22
Número de páginas	17
Revista	ACS Infectious Diseases
Volume	7
Número de emissão	1
DOIs	https://doi.org/10.1021/acsinfecdis.9b00507
Estado da publicação	???researchoutput.status.published??? - 8 jan. 2021

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Cadima-Couto, I., Tauzin, A., Freire, J. M., Figueira, T. N., Silva, R. D. M., Pérez-Peinado, C., Cunha-Santos, C., Bártolo, I., Taveira, N., Gano, L., Correia, J. D. G., Goncalves, J., Mammano, F., Andreu, D., Castanho, M. A. R. B., & Veiga, A. S. (2021). Anti-HIV-1 Activity of pepRF1, a Proteolysis-Resistant CXCR4 Antagonist Derived from Dengue Virus Capsid Protein. ACS Infectious Diseases, 7(1), 6-22. https://doi.org/10.1021/acsinfecdis.9b00507

@article{b29cdd3112734678821d16d3088f898c,

title = "Anti-HIV-1 Activity of pepRF1, a Proteolysis-Resistant CXCR4 Antagonist Derived from Dengue Virus Capsid Protein",

abstract = "There is an urgent need for the development of new anti-HIV drugs that can complement existing medicines to be used against resistant strains. Here, we report the anti-HIV-1 peptide pepRF1, a human serum-resistant peptide derived from the Dengue virus capsid protein. In vitro, pepRF1 shows a 50\% inhibitory concentration of 1.5 nM with a potential therapeutic window higher than 53{\^a}000. This peptide is specific for CXCR4-tropic strains, preventing viral entry into target cells by binding to the viral coreceptor CXCR4, acting as an antagonist of this receptor. pepRF1 is more effective than T20, the only peptide-based HIV-1 entry inhibitor approved, and excels in inhibiting a HIV-1 strain resistant to T20. Potentially, pepRF1 can be used alone or in combination with other anti-HIV drugs. Furthermore, one can also envisage its use as a novel therapeutic strategy for other CXCR4-related diseases.",

keywords = "CXCR4, HIV, antagonist, antiviral drugs, peptide",

author = "Iris Cadima-Couto and Alexandra Tauzin and Freire, \{Joa{\~o} M.\} and Figueira, \{Tiago N.\} and Silva, \{R{\'u}ben D.M.\} and Clara P{\'e}rez-Peinado and Catarina Cunha-Santos and In{\^e}s B{\'a}rtolo and Nuno Taveira and Lurdes Gano and Correia, \{Joa{\~o} D.G.\} and Joao Goncalves and Fabrizio Mammano and David Andreu and Castanho, \{Miguel A.R.B.\} and Veiga, \{Ana Salom{\'e}\}",

note = "Publisher Copyright: {\textcopyright} ",

year = "2021",

month = jan,

day = "8",

doi = "10.1021/acsinfecdis.9b00507",

language = "English",

volume = "7",

pages = "6--22",

journal = "ACS Infectious Diseases",

issn = "2373-8227",

publisher = "American Chemical Society",

number = "1",

}

Cadima-Couto, I, Tauzin, A, Freire, JM, Figueira, TN, Silva, RDM, Pérez-Peinado, C, Cunha-Santos, C, Bártolo, I , Taveira, N, Gano, L, Correia, JDG, Goncalves, J, Mammano, F, Andreu, D, Castanho, MARB & Veiga, AS 2021, 'Anti-HIV-1 Activity of pepRF1, a Proteolysis-Resistant CXCR4 Antagonist Derived from Dengue Virus Capsid Protein', ACS Infectious Diseases, vol. 7, n.º 1, pp. 6-22. https://doi.org/10.1021/acsinfecdis.9b00507

Anti-HIV-1 Activity of pepRF1, a Proteolysis-Resistant CXCR4 Antagonist Derived from Dengue Virus Capsid Protein. / Cadima-Couto, Iris; Tauzin, Alexandra; Freire, Joaõ M. et al.
Em: ACS Infectious Diseases, Vol. 7, N.º 1, 08.01.2021, p. 6-22.

Resultado de pesquisa: ???type-name??? › ???researchoutput.researchoutputtypes.contributiontojournal.article??? › revisão de pares

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AU - Cadima-Couto, Iris

AU - Tauzin, Alexandra

AU - Freire, Joaõ M.

AU - Figueira, Tiago N.

AU - Silva, Rúben D.M.

AU - Pérez-Peinado, Clara

AU - Cunha-Santos, Catarina

AU - Bártolo, Inês

AU - Taveira, Nuno

AU - Gano, Lurdes

AU - Correia, Joaõ D.G.

AU - Goncalves, Joao

AU - Mammano, Fabrizio

AU - Andreu, David

AU - Castanho, Miguel A.R.B.

AU - Veiga, Ana Salomé

PY - 2021/1/8

Y1 - 2021/1/8

N2 - There is an urgent need for the development of new anti-HIV drugs that can complement existing medicines to be used against resistant strains. Here, we report the anti-HIV-1 peptide pepRF1, a human serum-resistant peptide derived from the Dengue virus capsid protein. In vitro, pepRF1 shows a 50% inhibitory concentration of 1.5 nM with a potential therapeutic window higher than 53â000. This peptide is specific for CXCR4-tropic strains, preventing viral entry into target cells by binding to the viral coreceptor CXCR4, acting as an antagonist of this receptor. pepRF1 is more effective than T20, the only peptide-based HIV-1 entry inhibitor approved, and excels in inhibiting a HIV-1 strain resistant to T20. Potentially, pepRF1 can be used alone or in combination with other anti-HIV drugs. Furthermore, one can also envisage its use as a novel therapeutic strategy for other CXCR4-related diseases.

AB - There is an urgent need for the development of new anti-HIV drugs that can complement existing medicines to be used against resistant strains. Here, we report the anti-HIV-1 peptide pepRF1, a human serum-resistant peptide derived from the Dengue virus capsid protein. In vitro, pepRF1 shows a 50% inhibitory concentration of 1.5 nM with a potential therapeutic window higher than 53â000. This peptide is specific for CXCR4-tropic strains, preventing viral entry into target cells by binding to the viral coreceptor CXCR4, acting as an antagonist of this receptor. pepRF1 is more effective than T20, the only peptide-based HIV-1 entry inhibitor approved, and excels in inhibiting a HIV-1 strain resistant to T20. Potentially, pepRF1 can be used alone or in combination with other anti-HIV drugs. Furthermore, one can also envisage its use as a novel therapeutic strategy for other CXCR4-related diseases.

KW - CXCR4

KW - HIV

KW - antagonist

KW - antiviral drugs

KW - peptide

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U2 - 10.1021/acsinfecdis.9b00507

DO - 10.1021/acsinfecdis.9b00507

M3 - Article

C2 - 33319557

AN - SCOPUS:85099023671

SN - 2373-8227

VL - 7

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JO - ACS Infectious Diseases

JF - ACS Infectious Diseases

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Anti-HIV-1 Activity of pepRF1, a Proteolysis-Resistant CXCR4 Antagonist Derived from Dengue Virus Capsid Protein

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