2015
DOI: 10.1016/j.ejpb.2014.11.021
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Stealth anti-CD4 conjugated immunoliposomes with dual antiretroviral drugs – Modern Trojan horses to combat HIV

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Cited by 44 publications
(28 citation statements)
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“…Ramana et al . developed anti-CD4 modified liposomes loaded with nevirapine and saquinavir and evaluated them for cellular uptake and antiretroviral responses in Jurkat T cell lines [50]. The liposomes were prepared by thin film hydration and covalently linked to anti-CD4 antibody via thiol-maleimide chemistry.…”
Section: Targeted Deliverymentioning
confidence: 99%
See 1 more Smart Citation
“…Ramana et al . developed anti-CD4 modified liposomes loaded with nevirapine and saquinavir and evaluated them for cellular uptake and antiretroviral responses in Jurkat T cell lines [50]. The liposomes were prepared by thin film hydration and covalently linked to anti-CD4 antibody via thiol-maleimide chemistry.…”
Section: Targeted Deliverymentioning
confidence: 99%
“…To such ends, short palindromic repeat (CRISPR)-associated protein-9 nuclease (Cas9) systems were developed for HIV-1 proviral excision in order to eliminate latent provirus [87, 88]. The means to deliver this cargo to lymphoid tissues such as GALT and lymph nodes as well as the CNS and specifically to CD4+ T cells and macrophages is being sought [49, 50, 53, 59]. Certainly the needs to develop novel polymer and medicinal chemistry approaches for optimal manufacture of receptor-targeted nanoformulated Cas9 is of utmost importance and inevitably to use such approaches to efficiency use such formulations in reducing provirus DNA in infected cell reservoirs of virus.…”
Section: Excision and Elimination Of Hiv Proviral Dnamentioning
confidence: 99%
“…Over 100 publications, most focused on particular types of cancer cells, show that targeted immunoliposomes improve the cell-type specificity of drug delivery and reduce toxicity. Therapeutic drug loaded immunoliposomes include those targeting cells expressing the VEGF-Receptors-2 and −3 (24), the oxytocin receptor(25), the epidermal growth factor receptor, EGFR (26), CD4 (27), and HER2 (28, 29). The active delivery of immunoliposomes generally improves cell-type specificity and drug effectiveness by 3- to 10-fold (25, 30, 31) over passive delivery.…”
Section: Introductionmentioning
confidence: 99%
“…The hypothesized delivery mechanism involved the interaction of the nanoformulation with membrane CD4, followed by its endocytosis, and pH-dependent endosomal escape of indinavir into the cell cytoplasm, where it inhibits the viral protease [70]. Very recently, a stealth anti-CD4-targeted immunoliposome loaded with saquinavir and nevirapine has been developed which demonstrated an efficient uptake of the drugs into CD4+ Jurkat T cells and an enhanced anti-viral efficacy at significantly lower concentrations when compared to the free drug [71]. Kovochich and colleagues designed lipid nanoparticles loaded with bryostatin-2, a protein kinase C activator able to activate latent HIV-1 infections.…”
Section: Nano-delivery Of Arvs To the Cellular Sanctuariesmentioning
confidence: 99%
“…In this context, the most studied sanctuary [71] saquinavir nevirapine CD4+ Jurkat T cells lipid NP-bryostatin-2 [72] nelfinavir CD4+ T-cells and in vivo model glycine/mannose-PPI [73] efavirenz monocytes/macrophages tuftsin-PPI [74] efavirenz macrophages mannose-PPI [75] lamivudine macrophages…”
Section: Central Nervous Systemmentioning
confidence: 99%