Chemokine Analogues Show Suitable Stability for Development as Microbicides

Cerini, Fabrice; Landay, Alan; Gichinga, Carolyne; Lederman, Michael M.; Flyckt, Rebecca; Starks, David; Offord, Robin E.; Gal, François Le; Hartley, Oliver

doi:10.1097/qai.0b013e31818c953f

Cited by 32 publications

(32 citation statements)

References 21 publications

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“…However, because of its strong CCR5 agonist activity that might induce local inflammation and because of the high production costs, the development of PSC-RANTES as a microbicide was stopped and efforts were put in finding recombinant analogues that retained the high potency and lacked the cellular activation associated with PSC-RANTES. Of these, 5P12-RANTES has the most interesting profile [186,187]; it combines very potent activity against a broad range of HIV subtypes, lacks signalling activity, does not induce CCR5 receptor sequestration and can be produced at low cost. More recent studies in Rhesus macaques showed complete protection by 5P12-RANTES against vaginal challenge with a SHIV [188].…”

Section: Entry/fusion Inhibitorsmentioning

confidence: 99%

HIV sexual transmission and microbicides

Ariën

Jespers

Vanham

2011

Reviews in Medical Virology

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Pathogens often rely on the contacts between hosts for transmission. Most viruses have adapted their transmission mechanisms to defined behaviours of their host(s) and have learned to exploit these for their own propagation. Some viruses, such as HIV, the human papillomavirus (HPV), HSV-2 and HCV, cause sexually transmitted infections (STIs). Understanding the transmission of particular viral variants and comprehending the early adaptation and evolution is fundamental to eventually inhibiting sexual transmission of HIV. Here, we review the current understanding of the mechanisms of sexual transmission and the biology of the transmitted HIV. Next, we present a timely overview of candidate microbicides, including past, ongoing and future clinical trials of HIV topical microbicides.

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Section: Entry/fusion Inhibitorsmentioning

confidence: 99%

HIV sexual transmission and microbicides

Ariën

Jespers

Vanham

2011

Reviews in Medical Virology

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“…In a complementary effort, antibodies (7, 148) and therapeutic nucleotides (35, 53, 95) are pursued as agents targeting chemokines. With all of these agents, oral availability is out of question; however, various approaches to improving metabolic stability have been successful (18, 95). In combination with the ample potential for optimization of receptor inhibition properties, this suggests that biologics and biomimetics may become a promising next generation class of therapeutics targeting the chemokine receptor system.…”

Section: On Druggability Of Chemokine Receptorsmentioning

confidence: 99%

What Do Structures Tell Us About Chemokine Receptor Function and Antagonism?

Kufareva

Gustavsson

Zheng

et al. 2017

Annu. Rev. Biophys.

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Chemokines and their cell surface G protein-coupled receptors are critical for cell migration not only in many fundamental biological processes but also in inflammatory diseases and cancer. Recent X-ray structures of two chemokines complexed with full-length receptors provide unprecedented insight into the atomic details of chemokine recognition and receptor activation, and computational modeling informed by new experiments leverages these insights to gain understanding of many more receptor:chemokine pairs. In parallel, chemokine receptor structures with small molecules reveal complicated and diverse structural foundations of small molecule antagonism and allostery, highlight inherent physicochemical challenges of receptor:chemokine interfaces, and suggest novel epitopes that can be exploited to overcome these challenges. The structures and models promote unique understanding of chemokine receptor biology, including the interpretation of two decades of experimental studies, and will undoubtedly assist future drug discovery endeavors.

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“…Griffithsin (Grft) is a lectin derived from red alga 16 that binds the HIV envelope glycoprotein gp120 and is among the most potent lectin inhibitor of HIV as well as exhibiting effectiveness against other enveloped viruses including SARS and Hepatitis C 17,18 . Both 5P12-RANTES and Grft have been shown to have properties suitable for microbicidal use, including stability over a wide pH range and inexpensive production in large quantities [19][20][21][22] . Furthermore, chimeras formed by fusing 5P12-RANTES or Grft with the HIV gp41-derived C-peptide C37 via a covalent linkage, namely 5P12-RANTES-L-C37 and Grft-L-C37, have consistently shown even higher potency and wider breadth of inhibition than the original proteins 23,24 .…”

Section: Introductionmentioning

confidence: 99%

“…These proteins were selected based on a combination of properties, including high potency to broadly neutralize many strains of HIV, and experimentally determined suitability as HIV microbicides 19,22 . SF disks are expected to be amenable to users, with easy insertion, followed by release of inhibitor in response to the body's own moisture.…”

Section: Introductionmentioning

confidence: 99%

Stabilization and Sustained Release of HIV Inhibitors by Encapsulation in Silk Fibroin Disks

Zhang

Herrera

Coburn

et al. 2017

ACS Biomater. Sci. Eng.

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Topical microbicides have the potential to provide effective protection against sexual transmission of HIV. Challenges in developing microbicides include their application in resource-poor settings with high temperatures and a lack of refrigeration, and low user adherence to a rigorous daily regimen. Several protein-based HIV inhibitors show great promise as microbicides, being highly specific and not expected to lead to resistance that would affect the efficacy of current antiretroviral treatments. We show that four potent protein HIV inhibitors, 5P12-RANTES, 5P12-RANTES-L-C37, Grft, and Grft-L-C37 can be formulated into silk fibroin (SF) disks and remain functional for 14 months at 25, 37, and 50 °C. These HIV inhibitor-encapsulated SF disks show excellent inhibition properties in PBMC and in human colorectal and cervical tissue explants, and do not induce inflammatory cytokine secretion. Further, the SF provides a mechanically robust matrix with versatile material formats for this type of application. Finally, a formulation was developed to allow sustained release of functional Grft for 4 weeks at levels sufficient to inhibit HIV transmission. This work establishes the suitability of HIV inhibitor-encapsulated SF disks as topical HIV microbicides that can be further developed to allow easy insertion for extended protection.

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Chemokine Analogues Show Suitable Stability for Development as Microbicides

Cited by 32 publications

References 21 publications

HIV sexual transmission and microbicides

HIV sexual transmission and microbicides

What Do Structures Tell Us About Chemokine Receptor Function and Antagonism?

Stabilization and Sustained Release of HIV Inhibitors by Encapsulation in Silk Fibroin Disks

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