A pharmaceutical Study on Anti-Gout Drug / (رقم التسجيلة. 179372)

تفاصيل مارك
000 -LEADER
fixed length control field	08959namaa22004451i 4500
003 - CONTROL NUMBER IDENTIFIER
control field	EG-GICUC
005 - أخر تعامل مع التسجيلة
control field	20260423121329.0
008 - FIXED-LENGTH DATA ELEMENTS--GENERAL INFORMATION
fixed length control field	260411s2025 ua a\|\|\|frm\|\|\| 000 0 eng d
040 ## - CATALOGING SOURCE
Original cataloguing agency	EG-GICUC
Language of cataloging	eng
Transcribing agency	EG-GICUC
Modifying agency	EG-GICUC
Description conventions	rda
041 0# - LANGUAGE CODE
Language code of text/sound track or separate title	eng
Language code of summary or abstract	eng
--	ara
049 ## - Acquisition Source
Acquisition Source	Deposit
082 04 - DEWEY DECIMAL CLASSIFICATION NUMBER
Classification number	‪615.4
092 ## - LOCALLY ASSIGNED DEWEY CALL NUMBER (OCLC)
Classification number	‪615.4
Edition number	21
097 ## - Degree
Degree	M.Sc
099 ## - LOCAL FREE-TEXT CALL NUMBER (OCLC)
Local Call Number	Cai01.08.08.M.Sc.2025.Ho.P
100 0# - MAIN ENTRY--PERSONAL NAME
Authority record control number or standard number	Hossam Abdo Ashour AbdelSamad,
Preparation	preparation.
245 12 - TITLE STATEMENT
Title	A pharmaceutical Study on Anti-Gout Drug /
Statement of responsibility, etc.	by Hossam Abdo Ashour Abdel Samad ; Supervision Prof. Dr. Mohamed Ahmed El-Nabarawi, Prof. Dr. Mahmoud Hassan Teaima, Dr. Samar Fathy El-Habal.
246 15 - VARYING FORM OF TITLE
Title proper/short title	دراسة صيدلية علي عقار للنقرس
264 #0 - PRODUCTION, PUBLICATION, DISTRIBUTION, MANUFACTURE, AND COPYRIGHT NOTICE
Date of production, publication, distribution, manufacture, or copyright notice	2025.
300 ## - PHYSICAL DESCRIPTION
Extent	141 pages :
Other physical details	illustrations ;
Dimensions	25 cm. +
Accompanying material	CD.
336 ## - CONTENT TYPE
Content type term	text
Source	rda content
337 ## - MEDIA TYPE
Media type term	Unmediated
Source	rdamedia
338 ## - CARRIER TYPE
Carrier type term	volume
Source	rdacarrier
502 ## - DISSERTATION NOTE
Dissertation note	Thesis (M.Sc)-Cairo University, 2025.
504 ## - BIBLIOGRAPHY, ETC. NOTE
Bibliography, etc. note	Bibliography: pages 119 -129.
520 #3 - SUMMARY, ETC.
Summary, etc.	Objective of this study was to design, optimize, and evaluate microneedle (MN)-based transdermal delivery systems for the management of gouty arthritis using febuxostat (FBX), either alone or in combination with lornoxicam (LRX). The study aimed to overcome the key limitations of conventional oral formulations of FBX and LRX, including poor aqueous solubility, moderate bioavailability, and systemic adverse effects. This combination enhances the bioavailability of drugs and improves patient compliance compared to traditional tables and gels. Furthermore, it ensures the optimal release kinetics of the drugs. The bioavailability of the Microneedle was evaluated In-Vivo.<br/>Gouty arthritis is characterized by an initial inflammatory reaction caused by monosodium urate (MSU) crystals formed in the joints and periarticular tissues. Febuxostat (FBX) is a BCS class II selective xanthine oxidase inhibitor that has a moderate F value (<49%), high permeability, and low solubility. This work created and tested a transdermal delivery system for FBX using chitosan nanoparticles (FBX-Ch NPs) embedded in PVP/Eudragit microneedles (MNs) for the treatment of gout. The optimized MN formulation (M1) displayed good mechanical strength, penetration depth (up to 7 layers of Parafilm), and controlled disintegration after 48 hours. In vitro release was nearly 100% within 48 hours, compared to 55% for pure FBX. <br/>Gouty arthritis is defined by an acute inflammatory response triggered by monosodium urate (MSU) crystals deposited in the joints and periarticular tissues. Febuxostat (Feb), a selective xanthine oxidase inhibitor, belongs to BCS class II, showing low solubility and high permeability with a moderate F value (<49%). Lornoxicam (LRX) is a potent nonsteroidal anti-inflammatory drug (NSAID) used extensively to manage pain and inflammatory conditions. However, the drug possesses poor aqueous solubility (i.e., BCS class II). This study presents a microneedle (MN) patch for the co-delivery of Febuxostat and Lornoxicam to tackle the challenges associated with gouty arthritis treatment. The optimized microneedle patch with a biodegradable polyvinyl alcohol (PVA)/polyvinylpyrrolidone(PVP), polyethylene glycol (PEG 400) matrix and chitosan backing worked well both in vitro and in vivo. Lornoxicam and Febuxostat were released at 99% and 100%, respectively, in vitro, within 48 hours. The microneedles were strong enough to withstand 1000g but disintegrated within minutes of skin contact<br/>In this chapter, In vivo evaluation in hyperuricemia-induced rat models revealed effective normalization of serum uric acid levels, restoration of xanthine oxidase activity, and marked suppression of inflammatory mediators including NF-κB, TNF-α, IL-1β, and VEGF. Histopathological examinations further confirmed substantial recovery of joint and hepatic architecture, characterized by reduced inflammation, fibrosis, and vascularization. Collectively, these findings establish microneedle technology as a non-invasive, patient-friendly, and superior alternative to conventional oral and topical formulations, offering enhanced bioavailability, sustained therapeutic action, and reduced systemic side effects in the management of gouty arthritis. <br/>Ex vivo permeation approached 110 µg/cm² versus 20 µg/cm² for pure FBX. Kinetic modeling revealed non-Fickian diffusion (n = 0.62, R² = 0.991), implying drug diffusion and polymer relaxation. In vivo, microneedle technology effectively normalized blood uric acid levels (**p < 0.0001), reinstated xanthine oxidase activity to baseline, and significantly reduced inflammatory indicators such as NF-κB, IL-1β, TNF-α, and VEGF. In vivo, microneedle technology effectively normalized blood uric acid levels (**p < 0.0001), reinstated xanthine oxidase activity to baseline, and significantly reduced inflammatory indicators such as NF-κB, IL-1β, TNF-α, and VEGF. Histopathological examinations of the joints and liver revealed nearly full recovery, characterized by little fibrosis, inflammation, and vascularization. This surpassed the effects of oral FBX and FBX-Ch NPs. <br/>In vivo studies utilizing a hyperuricemia rat model demonstrated that the microneedle patch decreased serum uric acid levels by 85.4% and inhibited xanthine oxidase activity in the serum and liver by 72.4% and 68.3%, respectively. The patch significantly reduced inflammatory markers like MMP-3, CRP, TNF-α, and IL-1β, demonstrating its anti-inflammatory properties. Histopathological analysis showed greater joint and hepatic architecture restoration and inflammation reduction than conventional formulations
520 #3 - SUMMARY, ETC.
Summary, etc.	يُعَدّ النقرس المفصلي أحد الأمراض الالتهابية المزمنة الناتجة عن تراكم بلورات اليورات أحادية الصوديوم (MSU) داخل المفاصل والأنسجة المحيطة بها، مما يؤدي إلى نوبات من الالتهاب الحاد، وارتفاع مستويات حمض اليوريك في الدم، وإحداث تغيرات مرضية في أنسجة المفاصل والكبد. وعلى الرغم من توافر بعض العلاجات التقليدية مثل عقار فيبوكسوستات (FBX) الذي يعمل كمثبط انتقائي لإنزيم الزانثين أوكسيديز، وعقار لورنوكسيكام (LRX) الذي يُعَدّ من مضادات الالتهاب غير الستيرويدية (NSAIDs)، إلا أن استخدامهما عبر الطرق الفموية التقليدية يواجه تحديات كبيرة، أهمها ضعف الذوبان المائي، وانخفاض التوافر الحيوي (<49%)، وظهور آثار جانبية جهازية قد تحد من فعاليتهما العلاجية.<br/>تهدف هذه الدراسة إلى تصميم وتطوير أنظمة حديثة لتوصيل الدواء عبر الجلد باستخدام تقنية الإبر المجهرية الذائبة (Microneedles) لتحسين فعالية العلاج وتقليل مخاطره. حيث تم تطوير نوعين من التراكيب: الأول يعتمد على تحميل FBX في صورة جسيمات نانوية باستخدام بوليمر الشيتوزان (FBX-Ch NPs) ثم دمجها داخل إبر مجهرية مكونة من بولي فينيل بيروليدون (PVP) وإيودراجيت (Eudragit). أما النوع الثاني فقد اعتمد على تصميم لصقة إبر مجهرية ثنائية الدواء لتحميل كل من FBX و LRX داخل مصفوفة من PVA/PVP مع PEG400، مع استخدام الشيتوزان كدعامة خلفية.<br/>تم تقييم خصائص هذه التراكيب من خلال دراسات في المختبر (In vitro) والتي أظهرت انطلاقًا شبه كامل للأدوية (99–100%) خلال 48 ساعة، مقارنة بانطلاق محدود للعقار الخام.
530 ## - ADDITIONAL PHYSICAL FORM AVAILABLE NOTE
Issues CD	Issues also as CD.
546 ## - LANGUAGE NOTE
Text Language	Text in English and abstract in Arabic & English.
650 #0 - SUBJECT ADDED ENTRY--TOPICAL TERM
Topical term or geographic name entry element	Pharmaceutical industry.
650 #0 - SUBJECT ADDED ENTRY--TOPICAL TERM
Topical term or geographic name entry element	صناعة الأدوية
653 #1 - INDEX TERM--UNCONTROLLED
Uncontrolled term	Microneedles
--	Gouty arthritis
--	polyvinyl pyrrolidone-K90
--	Eudragit RS D30
--	Febuxostat
--	Sustained release
--	Chitosan
--	Lornoxicam
--	xanthine oxidase activity
--	الإبر المجهرية
--	التهاب المفاصل النقرسي
700 0# - ADDED ENTRY--PERSONAL NAME
Personal name	Mohamed Ahmed El-Nabarawi
Relator term	thesis advisor.
700 0# - ADDED ENTRY--PERSONAL NAME
Personal name	Mahmoud Hassan Teaima
Relator term	thesis advisor.
700 0# - ADDED ENTRY--PERSONAL NAME
Personal name	Samar Fathy El-Habal
Relator term	thesis advisor.
900 ## - Thesis Information
Grant date	01-01-2025
Supervisory body	Mohamed Ahmed El-Nabarawi
--	Mahmoud Hassan Teaima
--	Samar Fathy El-Habal
Universities	Cairo University
Faculties	Faculty of Pharmacy
Department	Department of Pharmaceutics & Industrial Pharmacy
905 ## - Cataloger and Reviser Names
Cataloger Name	Shimaa
Reviser Names	Eman Ghareb
942 ## - ADDED ENTRY ELEMENTS (KOHA)
Source of classification or shelving scheme	Dewey Decimal Classification
Koha item type	Thesis
Edition	21
Suppress in OPAC	No

المقتنيات
Source of classification or shelving scheme	Home library	Current library	Date acquired	Inventory number	Full call number	Barcode	Date last seen	Effective from	Koha item type
Dewey Decimal Classification	المكتبة المركزبة الجديدة - جامعة القاهرة	قاعة الرسائل الجامعية - الدور الاول	11.04.2026	93729	Cai01.08.08.M.Sc.2025.Ho.P	01010110093729000	11.04.2026	11.04.2026	Thesis

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A pharmaceutical Study on Anti-Gout Drug / (رقم التسجيلة. 179372)