TY  - BOOK
AU  - Eman Mohamed Abd-Elmonem Bedir, 
AU  - Amna Mohamad AwadAllah Makky 
AU  - Wessam Hamdy Abd El-salam
AU  - Islam Ahmed Hamed Khalil 
TI  - A Pharmaceutical Study on Certain Topical  Formulations of an Antifungal Drug   / : Remainder of title / 
U1  - 615.4 
PY  - 2024///
KW  - Pharmaceutical Sciences and Drug Manufacturing
KW  - qrmak
KW  - Corneal targeting
KW  - Amorolfine HCl
KW  - Mixed micelles
KW  - Histopathology
KW  - Microbiological studies, and In vivo studies
N1  - Thesis (M.Sc.) -Cairo University, 2024.; Bibliography: pages 76-96; Issued also as CD
N2  - Fungal keratitis, another name for keratomycosis, is a serious and challenging condition that affects the eye and can result in irreparable vision loss or even blindness. Fungal infections in the eyes are mostly caused by the species of candida, which requires long-term usage of antifungal medication for therapy. 

Topical eye drops are the most convenient dosage form for treating keratomycosis because they are easy to apply and have good patient compliance when compared to other ocular dose forms. However, the complex anatomy of the eye makes it difficult to achieve adequate ocular drug concentration, reducing fungal infection clearance; thus, poor ocular bioavailability, limited retention time, and low ocular tissue penetration are major concerns in the topical use of antifungal agents.

Amorolfine hydrochloride (AMO) is a morpholine derivative with a broad-spectrum antifungal medication that has been used to treat a variety of human fungal infections brought on by yeasts, dermatophytes, and opportunistic pathogenic fungi.

Mixed micelles (MMs) have been chosen as potential nanocarriers for enhancing the corneal penetration and deposition of AMO. 

Optimum AMO-MMs showed enhanced antifungal activity with no irritation signs. AMO-MMs could be a promising alternative to the standard commercial ophthalmic suspension for fungal keratitis.

This study aimed to investigate and prove amorolfine HCl (AMO) antifungal activity upon drug encapsulation into a mixed micelles (MMs) vesicle system to uphold ocular penetration and drug activity. 

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