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Diagnostic Study Orient Water Services Pvt Ltd. Industrial Water Treatment Chemicals [Mba Programme]

Thesis Info

Author

Mashkoor, Asim

Supervisor

Sarfraz Mahmood Kakar

Department

University of Management and Technology

Program

MBA

Institute

University of Management and Technology

Institute Type

Private

City

Lahore

Province

Punjab

Country

Pakistan

Thesis Completing Year

2001

Thesis Completion Status

Completed

Page

97 .

Subject

Economics

Language

English

Other

Report presented in part requirement MBA final Advisor : Sarfraz mahmood Kakar; EN; Call No: TP 333.9123 MAS-D

Added

2021-02-17 19:49:13

Modified

2023-02-17 21:08:06

ARI ID

1676712776843

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28. Al-Qasas/The Narratives

28. Al-Qasas/The Narratives

I/We begin by the Blessed Name of Allah

The Immensely Merciful to all, The Infinitely Compassionate to everyone.

28:01
a. Ta. Sin. Mim.

28:02
a. These are the Messages of the Clear Book - The Divine Qur’an.

28:03
a. WE are going to recount to you some of the narratives of Moses and Pharaoh truthfully, for a people who believe.

28:04
a. Indeed, Pharaoh exalted himself in the land of Egypt, and
b. divided its citizens into different ethnic and social factions,
c. seeking to oppress one faction among them - Descendants of Jacob – and depriving them of all human rights and civil liberties,
d. and, slaughtering their baby-boys at birth, while sparing their women/baby-girls.
e. He - Pharaoh - was truly of the oppressors and tyrants.

28:05
a. However, WE wanted to empower those very people who were being oppressed in the land
of Egypt – Descendants of Jacob, and
b. to make them the leaders and to make them the inheritors.

28:06
a. And to empower them in the land by giving them political power and religious authority,
b. and to show Pharaoh and Haman and their armies - through them - the very thing that they had dreaded - and trying to prevent.

28:07
a. And so when Moses was born, WE inspired Moses’ mother by saying that:
b. ‘Keep breast feeding him as usual, but when you fear for his life, then put him afloat into the River Nile,
c. and, once you have done so, then do not fear and do not grieve for he will be saved.
d. Surely WE...

بائبل اور اسلام کی روشنی میں عورت کا مقام اور کردار

Status and role of  woman has been discussed in almost every religion. A considerable portion of the  Scriptures of  Sematic religions  also addressed issues regarding woman in one way or another. In the light of the teachings of the Bible Woman is a  sign of sin, cleverness, social injustice and  violence. On the other hand Islam gave  woman more recognition and freedom of choice regarding   marriage, , education, inheritance,   etc. Islam believes in the equality of  male and female and as a result in Islamic society  woman has been  enjoying a better status and position. In this article a comparison of the role and status  of a woman has been discussed in the light of Bible and Islam.

Identification of Prospective Inhibitor for Tryptophan Synthase to Combat Tuberculosis

The current study was aimed to identify new inhibitors against tryptophan synthase from Mycobacterium tuberculosis for anti-tuberculosis drug discovery. The α-subunit of tryptophan synthase being unique and unexplored protein target was selected for discovery of new inhibitors that can serve as leads for anti-TB drugs discovery with novel mode of action. Here a combination of computational and experimental approaches was utilized. Both the structure based (SB) and ligand based (LB) virtual screening approaches were employed for prediction and identification of new hits as inhibitors against α-subunit of tryptophan synthase from M. tuberculosis. The structure based virtual screening (SBVS) of eMolecules database was done against homology model for protein i.e., α-subunit of tryptophan synthase. Seven new inhibitors were identified on the basis of their binding score, binding interactions and physiochemical properties. Similarly, ligand based virtual screening (LBVS) was used for screening of “clean drug like” subset of ZINC database against pharmacophore model. This pharmacophore model was generated using the structures of already reported inhibitors of the α-subunit of TrpS from literature and hits were identified in terms of rmsd (<1). Later the molecular docking studies of hits into the active pocket resulted in identification of five new inhibitors against α-subunit of TrpS. The anti-tuberculosis activity of proposed inhibitors identified through SBVS and LBVS was performed using agar dilution method and LJ media based method that resulted in identification of a new benzamide inhibitor and ZINC09150898. The benzamide inhibitor showed 100% growth inhibition of H37Rv strain of M. tuberculosis at 25 μg/mL and considerable anti-mycobacterial effect up to 6 μg/mL in whole cell based activity. The second new inhibitor i.e., ZINC09150898 showed antibacterial activity against H37Rv strain of M. tuberculosis at the concentration of 50 µg/mL (100% inhibition) and partial inhibition up to 12 µg/mL. The binding stability of both benzamide inhibitor and ZINC09150898 inside the binding pocket was further investigated through MD simulation studies involving RMSD, RMSF and secondary structure analysis that showed no major structural fluctuations in protein structure during the explored time scale. The current study can be further extended for enzyme based assay evaluation and could be considered as candidate for drug discovery against tuberculosis. In our attempt to find out new lead candidates for anti-tuberculosis drug discovery we performed in silico comparison of putative drug binding pockets of twelve essential metabolic enzymes from M. tuberculosis and other bacterial pathogens belonging to the ESKAPE group. The aim of this comparative analysis was to provide guidelines for the likelihood of transferability of the inhibitors from one species to another. In this comparison pathways other than tryptophan biosynthesis were investigated and the selection of targets was based on availability of the 3D-structure. Drug binding pockets of these essential enzymes from selected metabolic pathways that were conserved across ESKAPE pathogens, M. tuberculosis, M. smegmatis and E. coli were compared using their reported 3D structures and amino acid sequence alignment. This comparative analysis showed that drug binding pockets of these enzyme are mostly identical with good sequence identity (70-100 %) across different species used in this study suggesting that inhibitor designed for enzyme target of one species may have chances to inhibit same enzyme target in other species as well. This study suggested that antibiotics targeting enzyme of one pathogen might have similar inhibitory potential against other bacterial species as well if their binding pockets are conserved and can effectively help in design of new antibiotics against M. tuberculosis and ESKAPE pathogens as well as.