Effect of PEG coating on the Vitexin liposomes for Oral treatment of ALD / (Record no. 607922)

000 -LEADER
fixed length control field 02216nam a22001577a 4500
082 ## - DEWEY DECIMAL CLASSIFICATION NUMBER
Classification number 610
100 ## - MAIN ENTRY--PERSONAL NAME
Personal name Iqbal, Arfa
245 ## - TITLE STATEMENT
Title Effect of PEG coating on the Vitexin liposomes for Oral treatment of ALD /
Statement of responsibility, etc. Arfa Iqbal
264 ## - PRODUCTION, PUBLICATION, DISTRIBUTION, MANUFACTURE, AND COPYRIGHT NOTICE
Place of production, publication, distribution, manufacture Islamabad :
Name of producer, publisher, distributor, manufacturer SMME- NUST;
Date of production, publication, distribution, manufacture, or copyright notice 2022.
300 ## - PHYSICAL DESCRIPTION
Extent 56p.
Other physical details Soft Copy
Dimensions 30cm
500 ## - GENERAL NOTE
General note Vitexin a natural flavonoid, occasionally used in pharmaceutics due to its variety of medicinal<br/>effects and its roles in fat metabolism, hepatoprotection, and anticancer therapies. It has been<br/>rendered important for diseases leading to chronic liver disease, such as NASH/NAFLD,<br/>diabetes, cardiovascular ailments, and Liver cirrhosis. Recently, it has been administered in pure<br/>drug formulation, in combination with other chemicals, and nanoparticulate form mostly<br/>intravenously for various types of liver diseases. In its pure form it shows lower bioavailability<br/>due to its insolubility in aqueous environments and a lower rate of intestinal absorption. Since<br/>vitexin is known for its role in reducing and reversing the complications arising from<br/>decompensated liver cirrhosis, liposomal nanoparticles encapsulating vitexin were prepared by<br/>the ‘thin-film hydration’ process along with passive drug loading. Polyethylene glycol (PEG)<br/>coating of vitexin-loaded nanoparticles was used in the oral treatment of advanced liver disease<br/>in this research. Wistar rat models of intense liver injury was prepared and treated with vitexinloaded liposomal nanoparticles coated with PEG-1000 and PEG-2000. Histopathological,<br/>serological analysis and various other parameters observed and analyzed during and after the<br/>disease induction and completion of the treatment protocol presented better results and a possible<br/>reversal of liver cirrhosis when nanoparticles were coated with PEG-2000 in oral treatment.<br/>PEG-2000 also shows positive role in the oral administration to match the effectiveness of<br/>previously used vitexin-loaded nanoparticles for intravenous treatment of liver cirrhosis.
650 ## - SUBJECT ADDED ENTRY--TOPICAL TERM
Topical term or geographic name entry element MS Biomedical Sciences
700 ## - ADDED ENTRY--PERSONAL NAME
Personal name Supervisor : Dr. Nosheen Fatima Rana
856 ## - ELECTRONIC LOCATION AND ACCESS
Uniform Resource Identifier <a href="http://10.250.8.41:8080/xmlui/handle/123456789/31846">http://10.250.8.41:8080/xmlui/handle/123456789/31846</a>
942 ## - ADDED ENTRY ELEMENTS (KOHA)
Source of classification or shelving scheme
Koha item type Thesis
Holdings
Withdrawn status Permanent Location Current Location Shelving location Date acquired Full call number Barcode Koha item type
  School of Mechanical & Manufacturing Engineering (SMME) School of Mechanical & Manufacturing Engineering (SMME) E-Books 02/20/2024 610 SMME-TH-807 Thesis
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