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Liposomal drug delivery system from laboratory to clinic

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TLDR
Fungisome is effective in fungal infections resistant to fluconazole, conventional Amp B and in virgin and resistant cases of visceral leishmaniasis, and cheaper than the commercially available formulation of liposomal amphotericin B.
Abstract
The main objective of drug delivery systems is to deliver a drug effectively, specifically to the site of action and to achieve greater efficacy and minimise the toxic effects compared to conventional drugs. Amongst various carrier systems, liposomes have generated a great interest because of their versatility. Liposomes are vesicular concentric bilayered structures, which are biocompatible, biodegradable and nonimmumnogenic. They can control the delivery of drugs by targeting the drug to the site of action or by site avoidance drug delivery or by prolonged circulation of drugs. Amphotericin B (Amp B) remains the drug of choice in most systemic mycoses and also as a second line treatment for Kala azar. However, its toxic effects often limit its use. Although the liposome delivery system has been tried for several drugs, only a few have been used in patients due to the slow development of necessary large-scale pharmaceutical procedures. This paper reviews the development of the technique for liposomal Amphotericin B (L-Amp-LRC-1, Fungisome) drug delivery system in our laboratory in collaboration with the department of Biochemistry, Delhi University in India and proving the safety and efficacy of this preparation in clinical practice. It also attempts to compare the efficacy and benefits of our product for Indian patients with those of similar products and it includes facts from the publications that flowed from our work. As compared to conventional Amp B, Fungisome is infused over a much shorter period requiring a smaller volume and no premedication. It was found to be safe in patients who had developed serious unacceptable toxicity with conventional Amp B. In renal transplant patients, Fungisome did not produce any nephrotoxicity. Fungisome is effective in fungal infections resistant to fluconazole, conventional Amp B and in virgin and resistant cases of visceral leishmaniasis. The cost of any drug is of great significance, especially in India. We have therefore devoted a section of our review to the relative costs of our product and those of other commercially available products. This patient-worthy formulation is safe, efficacious and cheaper than the commercially available formulation of liposomal amphotericin B. The product has been patented and technology transferred to a pharmaceutical company for marketing. Results of postmarketing study also document safety and efficacy as observed in premarketing studies. A brief review of this work is provided here.

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Liposomes as delivery systems for antibiotics

TL;DR: In an era of an avalanche of increasing bacterial resistance and severe problems in treating bacterial infections, the application of liposomal antibiotic carriers could be useful, but the high cost ofliposome preparation and treatment should also be considered.
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Liposomal amphotericin B: a review of its use as empirical therapy in febrile neutropenia and in the treatment of invasive fungal infections.

TL;DR: Liposomal amphotericin B remains a first-line option for empirical therapy in patients with febrile neutropenia and in those with disseminated histoplasmosis, and is an option for the treatment of AIDS-associated cryptococcal meningitis, and for invasive Candida spp.
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Delivery of peptide and protein drugs over the blood-brain barrier.

TL;DR: This review combines a comprehensive overview on the current understanding of the transport mechanisms at the blood-brain barrier with promising selected strategies published so far that can be applied to facilitate enhanced P/P drug delivery over the BBB.
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Application of various types of liposomes in drug delivery systems

TL;DR: A new generation of liposomes is discussed, which is utilized for decreasing the limitation of the conventional liposome, and there are many factors and difficulties that affect the development ofliposome drug delivery structure.
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Delivery systems to increase the selectivity of antibiotics in phagocytic cells.

TL;DR: Recent advances and current perspectives in the use of antibiotic delivery systems in the treatment of intracellular infections such as mycobacterial infections, brucellosis, salmonellosis, listeriosis, fungal infections, visceral leishmaniasis, and HIV are analyzed.
References
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Journal ArticleDOI

Diffusion of Univalent Ions Across the Lamellae of Swollen Phospholipids

TL;DR: It is found that as the surface charge of the lipid lamellae is increased, the amount of cation per μmle of lipid increases, and the phospholipid liquid crystalline structures appear to “bind” or “capture” cations.
Journal ArticleDOI

Liposomal Amphotericin B for the Treatment of Systemic Fungal Infections in Patients with Cancer: A Preliminary Study

TL;DR: Twelve patients with hematologic malignancies complicated by fungal infections were treated with liposomal amphotericin B (L-AmpB); nine patients were granulocytopenic; the three additional patients with normal granulocyte counts were immunosuppressed.
Journal ArticleDOI

Amphotericin B: Time for a New “Gold Standard”

TL;DR: The cumulative clinical experience to date with the lipid-based preparations is now adequate to demonstrate that these agents are no less active than AmBD, and, for some infections, it can now be stated that specific lipid- based preparations of AmB are superior to AmBD.
Journal ArticleDOI

Treatment and Prophylaxis of Disseminated Infection Due to Candida albicans in Mice with Liposome-Encapsulated Amphotericin B

TL;DR: The encapsulated drug was as effective as the free drug when used in similar concentrations, while the animals treated with higher concentrations of liposomal amphotericin B had a longer survival time and an improved therapeutic index resulted by encapsulating amph esotericin B in liposomes.
Journal ArticleDOI

Treatment of Systemic Fungal Infections With Liposomal Amphotericin B

TL;DR: Liposomal amphotericin B therapy was effective and less toxic than conventional amphoteric in B therapy and no chronic renal, hematologic, or central nervous system side effects were observed.
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