Researcher Image
حنان جلال نعوم عبد الكريم - Hanan Jalal Kassab
PhD - assistant professor
College of pharmacy , Department of pharmaceuticals
[email protected]
Summary

PhD pharmacy pharmaceutics I graduated with an MSc degree in Pharmaceutics from the College of Pharmacy, University of Baghdad in 1999, with expertise in tabletting in pharmaceutical formulation, since then I have been working as an assistant lecturer in the Department of Pharmaceutics labs (Physical Pharmacy, Pharmaceutical Technology, Industrial Pharmacy) and then went to do a Ph.D. on the "5FU in-situ rectal gel " under the supervision of Prof. Yehya Ismail in 2012, since then I have being responsible for giving lectures in Pharmaceutics undergraduate studies as a lecturer and supervision of Diploma and MSc students and was promoted to Assistant Professor in 2019, I was given the responsibility of teaching and Supervision of PhD students.

Qualifications

BSc pharmacy 1993 College of Pharmacy University of Baghdad MSc pharmacy Pharmaceutics 1999 College of Pharmacy University of Baghdad PhD pharmacy pharmaceutics 2012 College of Pharmacy University of Baghdad

Research Interests

Pharmaceutics Pharmaceutical formulation I am interested in development (preparation formulation evaluation of pharmaceutical dosage forms), especially gels. Research in my laboratory mainly concentrated on different types of gels, including the in-situ gels, and method of preparation, in addition to other dosage forms concerning various types of polymers. The aim is to improve and develop appropriate palatable dosage forms.

Teaching materials
Material
College
Department
Stage
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pharmaceutical Technology
كلية الصيدلة
الصيدلانيات
Stage 3
Teaching

Teaching (undergraduate)  Physical Pharmacy I, II
 Pharmaceutical Technology I, II  Industrial Pharmacy II Teaching (postgraduate) • Quality Assurance Diploma • Absorption of Drugs Diploma • Selected topics Ph.D. level • Advanced Biopharmaceutics MSc level

Supervision

Preparation and evaluation of Naproxen In situ ocular pH-sensitive gel Preparation of sodium fusidate topical gel using different gelling agents Formulation and In-vitro Evaluation of Fexofenadine HCl as a Mucoadhesive Ophthalmic Gel Studying the Effect of Variables on Acyclovir Microsponge Preparation and In-Vitro Evaluation of Paromomycin as Dermal Film Preparation and In-Vitro Evaluation of Bromhexine HCl Oral Gummy Formulation and evaluation of preservative-free soluble granules of Salbutamol Sulphate Formulation and evaluation of sumatriptan as mucoadhesive in situ intranasal gel by using different thermosensitive polymers Enhancement of prednisolone solubility by complexation with β-cyclodextrin “Formulation and in - vitro evaluation of Bromhexine HCl lozenges” Preparation and in-vitro evaluation of Secnidazole as oral In-situ gel for treatment of periodontal disease Preparation and in-vitro Evaluation of Clotrimazole as Oral gel Preparation and in-vitro Evaluation of fast-dissolving film of Montelukast Sodium as Nipple Shield delivery Preparation And Evaluation of Topical Butenafine Hydrochloride Nanosponge Formulation and Evaluation of Clotrimazole vaginal foam Formulation and in vitro characterization of Nefopam HCl as mucoadhesive thermosensitive in situ nasal gel Preparation and Evaluation of Cilnidipine Nanoparticle as Oral Drug Delivery Diacerein novasome as transdermal drug delivery: formulation, in vitro, ex vivo characterization and in vivo study Brain Targeted Intranasal Delivery of In Situ Gel Loaded Frovatriptan Succinate Binary Ethosomes: Preparation, In-Vitro and In-Vivo Evaluation. Amisulpride Loaded Nanostructured Lipid Carriers Targeted Nose to Brain: Formulation and In-Vitro/ In-Vivo Study Invasomes Transdermal Gel Using Disulfiram as Modelling Drug: Preparation and In-vitro / In-vivo Study Preparation and Evaluation of Voriconazole as Topical Organogel

Publication Date
Mon Jan 01 2024
Journal Name
Nanotechnology, Science And Applications
Formulation and Characterization of Intranasal Drug Delivery of Frovatriptan-Loaded Binary Ethosomes Gel for Brain Targeting
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Background: Frovatriptan succinate (FVT) is an effective medication used to treat migraines; however, available oral formulations suffer from low permeability; accordingly, several formulations of FVT were prepared. Objective: Prepare, optimize, and evaluate FVT-BE formulation to develop enhanced intranasal binary nano-ethosome gel. Methods: Binary ethosomes were prepared using different concentrations of phospholipid PLH90, ethanol, propylene glycol, and cholesterol by thin film hydration and characterized by particle size, zeta potential, and entrapment efficiency. Furthermore, in-vitro, in-vivo, ex-vivo, pharmacokinetics, and histopathological studies were done. Results: Regarding FVT-loaded BE, formula (F9) demonstrated the best paramet

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Publication Date
Mon Jan 01 2024
Journal Name
Journal Of Research In Pharmacy
Cilnidipine Nanoparticles Oral Film: Preparation and Evaluation
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Cilnidipine is a dihydropyridine class of calcium channel blockers, it is classified as a BCS class II drug, characterized by a low oral bioavailability of 13%. Consequently, the utilization of nanoparticle preparation is anticipated to enhance its bioavailability. The objective of the research is to integrate cilnidipine nanoparticles into oral films as a means of enhancing patient adherence. The optimal polymers for producing Cilnidipine films were PVA cold and or HPMC E5 at different concentrations using a casting technique with glycerol as a plasticizer. The Nano suspension-based preparation of Cilnidipine's oral film containing the combination of polymers exhibited a significant enhancement in vitro dissolution, with a percentage excee

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Publication Date
Sun Jan 01 2023
Journal Name
Journal Of Advanced Pharmaceutical Technology & Research
Use of factorial design in formulation and evaluation of intrarectal in situ gel of sumatriptan
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Publication Date
Tue Nov 21 2023
Journal Name
Pharmacia
A comparative study of oral diacerein and transdermal diacerein as Novasomal gel in a model of MIA induced Osteoarthritis in rats
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Background: Osteoarthritis is a chronic pathology of the joints causing disability and morbidity. Diacerein is a disease-modifying agent indicated for osteoarthritis management with enhanced performance and have much lower side effects profile than conventional non-steroidal anti-inflammatory drugs. Oral administration of Diacerein is associated with a laxative effect, thus causing treatment discontinuation. Aim: This study aimed to evaluate the activity of Diacerein novasome-based transdermal gel compared with standard oral treatment in the management of induced osteoarthritis in a rat model. Materials and methods: A single intra-articular injection of monosodium iodoacetate was administered to the left knee joint, resulting in the develop

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Publication Date
Fri Nov 03 2023
Journal Name
Iraqi Journal Of Pharmaceutical Sciences( P-issn 1683 - 3597 E-issn 2521 - 3512)
Factors affecting the preparation of Cilnidipine nanoparticles
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Cilnidipine is a dihydropyridine calcium channel blocker used to improve the neurological outcome following subarachnoid hemorrhage. It belongs to BCS class II drugs that have a low oral bioavailability of 13%, thus preparation as nanoparticles would be expected to improve bioavailability. The aim of the study is to prepare Cilnidipine as nanoparticles using different carriers and co-carriers, concentrations, and types. Cilnidipine nanoparticles were prepared by a solvent anti-solvent method using different carriers (Soluplus®, Poloxamer 188, PVA cold) with co-stabilizers (PEG200, glycerol) at different ratios. Based on the obtained results, formula N4, which included Soloplus in a 5:5:1.19 weight ratio of drug to

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Publication Date
Fri Nov 03 2023
Journal Name
Iraqi Journal Of Pharmaceutical Sciences( P-issn 1683 - 3597 E-issn 2521 - 3512)
Diacerein Loaded Novasome for Transdermal Delivery: Prepartion , In-Vitro Characterization and Factors Affecting Formulation
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Diacerein (DCN) is a semi-synthetic anthraquinone derivative of Rhein that is indicated for the management of osteoarthritis. Diacerein exhibits poor dissolution in the GIT fluids and suffers from low bioavailability upon oral administration in addition to the laxative effect of Rhein metabolites. The aim of the present study was to develop novasomal vesicles with optimized entrapment efficiency and size to serve as a carrier for transdermal delivery of diacerein. Novasomal vesicles were prepared by thin film hydration method thin film hydration. The prepared vesicles were optimized utilizing different surfactant to cholesterol molar ration, sonication type, different sonication times and varying fatty acid level. The prepared vesicles were

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