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Mapping Genes Causing Postaxial Polydactyly

Thesis Info

Author

Bilal Khan

Supervisor

Wasim Ahmad

Department

Department of Biochemistry, QAU

Program

Mphil

Institute

Quaid-i-Azam University

Institute Type

Public

City

Islamabad

Province

Islamabad

Country

Pakistan

Thesis Completing Year

2016

Thesis Completion Status

Completed

Page

xv, 94

Subject

Biochemistry

Language

English

Other

Call No: DISS / M.PHIL / BIO/ 4303

Added

2021-02-17 19:49:13

Modified

2023-02-19 12:33:56

ARI ID

1676715744653

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اداریہ

سیالکوٹ کی تہذیب قدامت کے لحاظ سے پانچ ہزار سال سے بھی پہلے کے آثار ظاہر کرتی ہے۔راجہ شل نے اس تہذیب کو پروان چڑھانے میں اہم کردار ادا کیا۔اس شہر کی تہذیبی روایات اور علمی آثار " مہابھارت" میں بدرجہ اُتم موجود ہیں۔سیالکوٹ کی مٹی بڑی زرخیز اور مردم خیز ہے۔سرزمین سیالکوٹ نے علم وادب وفنون لطیفہ کے میدانوں میں گراں قدر خدمات سرانجام دی ہیں۔سیالکوٹ کی علمی وادبی  اہمیت مسلمہ ہے۔ہر دور میں خواہ وہ ہندو راج ہو ، مغلیہ راج ہویا انگریز راج سیالکوٹ نے ہردور میں علمی وادبی مرکز کے حوالے سے اپنی شناخت قائم رکھی ہے۔یہاں سے بہت سی نامور روحانی اور علمی وادبی شخصیات نے جنم لیا ہےاور بعض نے یہاں کی روحانی اور علمی وادبی شخصیات سے فیض حاصل کیا ہے۔٧٠٠ قبل مسیح سے٦٠٠ قبل مسیح تک یہ اتنا عظیم تعلیمی مرکز تھا۔کہ بنارس کے شہزادے حصول علم کے لیے یہاں آتے تھے۔

اکیسویں صدی عیسویں میں بھی شہرِ اقبال اپنی تہذیبی و ادبی  روایات کی بازیافت کے لیے خاصا سرگرم عمل ہے۔ملا عبدالحکیم سیالکوٹی ،مولانا فیروزالدین،اقبال ،فیض ،مولانا ظفر علی خاں،  ہاشم شاہ،حضرت رائج سیالکوٹی، دلشاد ،منشی میراں بخش جلوہ،محمد الدین فوق ،اثر صہبائی ،سلیم واحد سلیم ،بدری ناتھ سدرشن،جوگندر پال ،غلام الثقلین نقوی ،رجندر سنگھ بیدی،عبدالحمید عرفانی،سرمد صہبائی،خالد نظیر صوفی، ڈاکٹر جاوید اقبال،ساغر جعفری،مولوی ابراہیم میر،آسی ضیائی رامپوری،طفیل ہوشیارپوری،اے ڈی اظہر،حفیظ صدیقی،صابر ظفر،اصغر سودائی اور جابر علی سید دنیائے شعروادب کے اہم ستارے ہیں۔جن کا تعلق سیالکوٹ کی دھرتی کے ساتھ تادمِ حیات رہا ۔موجودہ دور میں بھی خطہ سیالکوٹ علمی وادبی میدان میں مضافاتی دائرے سے نکل کر قومی وبین الاقوامی ادبی دھارےمیں شامل ہونے کے لیے پرتول رہا ہے۔پنجاب لٹریری فورم سیالکوٹ اسی سلسلے میں اہم کردار ادا کررہا ہے۔اس ادبی تحریک کا ثمر اس خطے کی ادبی سرگرمیوں...

القاضي عياض: حياته وآرائه في علم الحديث

ABSTRACT: Qazi Ayaz was one of the great scholars in the Knowledge of Hadith. He enjoys a unique status in his memory, narration and understanding of Hadith. He has vast knowledge of chains of Hadith, its transmitters, and their biographies. For acquiring this high position he always travelled to get the Hadith from its well-known experts, and used utmost care in getting the authentic chains of transmitters, so much so that he is considered an authority among the great scholars ofHadith. The methodology of Ayaz in the science of the transmission of Hadith is based upon research, accuracy and authentication ofthe text. He considers the science of transmission and narration. The origin and essence in authenticating the Hadith. He was strict in the criticism of the text of Hadith and emphasized on the narration of the Prophet’s words instead of allowing the narration of the meanings, unlike the other scholars of Hadith. Hence he held some special views, due to his long experience in Hadith. Some of his views are about: The comparison with the original hearing. The appropriate age while transmitting Hadith toothers. The omitting ofrepeated words in Hadith. The usage of the marks of dialect in the text ofHadith. The permission in narration ofthose Hadith about which he himselfdoes not have permission

Immunodynamics of Hiv-1 in Genetically Diverse Cohorts

Under the influence of host immune pressures, human immunodeficiency virus (HIV) rapidly accumulates and selects mutations that confer survival advantage to the virus. The human leukocyte antigen (HLA) represents one of the major host selection pressures that drive the antigenic evolution of HIV. During the course of infection, the interplay of host and virus factors determines the eventual outcome of the disease as well as the repertoire of predominant viral mutants in a given host milieu. In global perspective, this cross-talk between the host and the virus is observed as population-specific amplification of particular HIV subtypes, recombinant forms, or mutation variants. This study focuses on the HIV immunogenic protein Gag to analyze; a) the association of host immunity and viral genetic variability with disease progression, b) HIV subtype A divergence and epitope evolution at global as well as at population level, and c) co-occurring epitope mutations in HIV Gag, using a new in-house bioinformatics tool. Methodology: In this study, a total of 1893 subtype A sequences, from mid-1980s to late 2000s, representing 19 different countries, were included for global analysis. For cohort study, 15 Afghan, 50 Kenyan and 74 Pakistani HIV positive samples were collected. Using a variety of bioinformatics software, the sequences from HIV-1 Gag region p24 and p2p7p1p6 were analyzed for mutations affecting genetic divergence and epitope evolution (predominantly V303 to T303 mutation in the Pakistani and Kenyan cohorts, respectively). Subsequently, the population-specific Gag mutations V303 and T303 were focused for in vitro analysis. Proteasomal assays followed by Mass Spectrometry were performed to evaluate the significance of V303 and T303 mutation in epitope processing. The HIV divergence was analyzed using phylogenetic networks and Bayesian Skyline plot, whereas, the genomic variability of Gag was measured in terms of GàA substitutions and Shannon entropy. Finally, a new Bioinformatics software, I-CAN (Identification of Co-occurring Amino acids and Nucleotides), was developed and used to analyze Gag epitope mutations co-occurring with the mutation V303T in Pakistani and Kenyan sequences. Results: In the Kenyan cohort, a linear trend between HIV genomic variability, and high viral load and low CD4 count was observed. Furthermore, certain Gag mutations unique to either Pakistani or Kenyan cohort were observed to affect the epitope processing in a population-specific manner. As a consequence of these mutations, epitope pattern in the two cohorts was uniquely altered. In the global analysis, it was observed that the HIV subtype A diverged around mid-90s from Kenya, exhibiting an upward trend in genomic variability that peaked in the last 5 years (2005-2010) of the analysis. A similar trend was also observed in Gag epitopes, where point mutations gave rise to novel Gag epitopes, evolving especially in the years 2005-2010. Finally, the results from the tool I-CAN, indicated a strong association in certain Gag co- occurring epitope mutations and the patient‟s HLA types. Conclusion: A pattern of population-specific Gag epitopes was observed that appeared to be evolving under selection pressures from the host HLA. Further investigation of these mutations will enhance the understanding of the evolution of HIV under host/population-specific selection pressures. This information may be helpful in designing vaccine and treatment strategies against HIV.