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Home > بدعت کے احکام و مراتب: الاعتصام للشاطبی کے باب خامس اور سادس کا تحقیقی و تحلیلی جائزہ۔

بدعت کے احکام و مراتب: الاعتصام للشاطبی کے باب خامس اور سادس کا تحقیقی و تحلیلی جائزہ۔

Thesis Info

Author

حنان عارف

Supervisor

مسعود قاسمحافظ

Program

MA

Institute

Riphah International University, Faisalabad

City

فیصل آباد

Degree Starting Year

2017

Language

Urdu

Keywords

فقہی مسائل , بدعات

Added

2023-02-16 17:15:59

Modified

2023-02-16 22:08:49

ARI ID

1676733240486

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قاری جلیل الرحمٰن عثمانی

عثمانی، قاری جلیل الرحمن
ایک ولی اﷲ کی وفات
قاری جلیل الرحمن عثمانی کاانتقال پرملال
دیوبند قصبہ میں جہاں حضرت مولانا قاسم نانوتویؒ نے علمِ دین کی شعاعیں تمام دنیامیں پھیلائیں اوردارالعلوم جیسا عظیم علمی دینی ادارہ قائم کرکے رہتی دنیا تک دیوبند کانام روشن کیا وہاں دیوبند قصبہ کوخود اس بات کاشرف و اعزاز حاصل ہے کہ اس کی سرزمین پرایسی ایسی نامور برگزیدہ جلیل القدر ہستیوں نے بھی جنم لیاجن کی بے پناہ خداداد صلاحیتوں کی بدولت اﷲ کے بندوں نے بہت کچھ علم وعمل اورروحانی فیوض وبرکات حاصل کیے۔سرزمین دیوبند میں حضرت مولانا قاری مفتی عزیزالرحمن عثمانیؒ کی ہستی ایسی تھی جنہیں لوگ ولی اﷲ کہتے تھے۔ان کے عمل وکردار نے کتنے ہی لوگوں کوراہ مستقیم دکھلائی ۔ہزاروں انسانوں نے ان کی پاکیزہ زندگی سے رہنمائی حاصل کی۔دیوبند کے علاوہ ہندوستان اور بیرونِ ممالک کے عوام نے ان کی روحانی ہستی کو سمجھا اور پہچانا۔ قدرتی بات ہے کہ ان کے خاندان میں ان کی روحانی برکت سے ان کی اولاد میں ان کی بہترین واعلیٰ دینی تربیت سے جواولاد پیدا ہوئی اس نے بھی اپنے نیک عمل وکردار کاوہ نقش قائم کیا جو قابل رہنما اصول ہے۔مفکرِ ملّت حضرت مفتی عتیق الرحمن عثمانیؒ بانی ادارہ ندوۃ المصنفین ورسالہ برہان اورحضرت قاری جلیل الرحمن عثمانی ؒ حضرت مولانا مفتی عزیز الرحمن عثمانیؒ کے لائق فرزند تھے۔ ۱۹۸۴ء میں مفکر ملّت مفتی عتیق الرحمن عثمانیؒ کی وفات ہوئی جس سے ملّت اسلامیہ کوناقابل تلافی نقصان پہنچا اوراب یکم ستمبر ۹۵ء کوحضرت مولانا مفتی عزیزالرحمن عثمانیؒ کے صاحبزادے اور مفکرِملّت مفتی عتیق الرحمن عثمانیؒ کے اکیلے برادر خوردحضرت قاری جلیل الرحمان عثمانی انتقال فرماگئے ۔انا ﷲ وانا الیہ راجعون۔
مرحوم بڑے ہی خوش خلق ملنسار اور باکمال روحانی اوصاف کے حامل انسان تھے۔حضرت مفتی عتیق الرحمن عثمانیؒ تو چھپے ہوئے ولی تھے۔ ان کی خوبیوں...

فن حدیث میں مولانا عبد الرحمن مبارک پوری کی خدمات کا جائزہ

Sūnan-ul-Tirmizi is an encyclopedia of Ahādith-ul-Ahkām. Imam Tirmizi is the Mohadith who divided hadiths into Sahih and Zaeef for the first time. He accepts or rejects a hadith on the base of Taāmul-e-Ummah. He is only the Mohadith who established the terminology of “Filbāb” in which he gives the words of hadith from a Sahabi and mentions the names of all other sahabies who are rawi of the same hadith. There are many sharh of Tirmizi written by Muhadiseen. Among them Tuhfat ul Ahwazi is famously written by Molana Abdul Rahman Mubarakpuri. He explores the terminologies of Sonan-e-Tirmizi. He discussed uloom ul hadith, books of hadith, Shoroh-ul-hadith, Asma-ul-rejal and ilm ul ansab etc. He mentions tafsiri aqwal, fiqhi problems and usool-e-hadith. He also solved the Tasaholat-e-Tirmizi in validity (sihat) and unvalidity (zouf). He is the first mohadith who tried to find the words of hadith from other sahabies whose names are given in “Filbab”. He did it but could not find the words of 87 ahadith for which he used the term “Lam aqif alaih” and 417 ahadith for which he used the term “Le Yonzar man akhraja haza ul hadith”. This thing makes it distinct from other shoroh of Sūnan-e-Tirmizi. He depends on the usool-e-hadith of forefather Muhadiseen and he did not establish his own usool hadith.

Linguistic Competence and Self Actualization of Pakistani Postgraduate Research Schoalrs in Psychosocial Perspectives.

The aim of any pharmaceutical dosage form designing is to formulate a product that not only provide the desired therapeutic responses but improve patient satisfaction too. For this purpose, modification in the existing dosage forms has been continued through alteration of additives and the optimization of manufacturing technique to achieve targets. Controlled release (CR) formulations have ability to maintain plasma drug concentration within the therapeutic range for longer duration of time resulting in reduced dosing. The goal of the present study was to prepare once daily valsartan CR 160 mg tablets using swellable hydrophilic and hydrophobic polymers to reduce the fluctuation in plasma level and to sustain steady state over an extended time. Being angiotensin-II receptor blocker, commonly prescribed to manage hypertension. It can also be used in patients of heart failures who cannot tolerate ACE inhibitors or others. Valsartan is commonly prescribed for treatments of left ventricular hypertrophy, isolated systolic hypertension and diabetic nephropathy. Moreover, it is considered an alternative drug to treat myocardial infarction, heart failure, coronary artery disease and systolic dysfunction. In this study different hydrophobic and hydrophilic polymers were utilized to develop valsartan controlled release formulations. They included Methocel® K4M (K4M1- K4M9), K15M (K15M1-K15M9) & K100M (K100M1-K100M9), Ethocel® Standard 7 FP (E7FP1-E7FP9), Kollidon® SR (KSR1- KSR9) and blend of Methocel® K4M & Kollidon® SR (K4M : KSR1-K4M : KSR20). These polymers were used in different concentrations to observe their influence on drug release. Each formulation contained valsartan, rate controlling polymer, Avicel PH 101 and magnesium stearate. Total sixty-five valsartan SR formulations were prepared by CCRD using software Design Expert® (ver. 7.0.). Drug-excipient compatibilities were determined using Fourier transformed-infrared spectroscopy (FT-IR) and no interactions were found between valsartan and various formulation excipients. Powder blend properties (Hausner ratio, compressibility index and angle of repose) and compressed tablets evaluation (weight variation, thickness, hardness and friability) were carried out and found to be satisfactory for formulations of Methocel® K4M (K4M2, K4M3, K4M9), Methocel® K15M (K15M3, K15M6, K15M9), Methocel® K100M (K100M2, K100M3, K100M5, K100M9), Ethocel® Standard 7 FP Premium (E7FP2, E7FP3, E7FP9), Kollidon® SR (KSR2, KSR3, KSR9) and blend of Methocel® K4M & Kollidon® SR formulations (K4M : KSR1, K4M : KSR2, K4M : KSR5, K4M : KSR11, K4M : KSR12, K4M : KSR18 and K4M : KSR20). All trial valsartan formulations were assayed using a validated spectrophotometric and HPLC methods at wavelength of 250 and 264 nm respectively. Assay results of all formulations were found within the official range of 95-105 %. In vitro dissolution of developed formulations were performed in different dissolution media including HCl pH 1.2, phosphate buffer pH 4.5 and 6.8. Desirable drug release profile was achieved by K4M9 formulation (25 % Methocel® K4M) which showed 23 %, 82 % and 100.16 % drug release in 4, 16 and 24 hrs respectively. Higher viscosity grades of Methocel® K15M (K15M3, K15M6 & K15M9) and K100M (K100M2, K100M3, K100M5 & K100M9) excessively sustained the release of valsartan. Excessive control on drug release was exhibited by hydrophobic Ethocel® based formulations (E7FP3 & E7FP9) at various concentrations not showing compliance with the criteria of CR formulation. Although KSR2 and KSR9 formulations of Kollidon® SR (25 % & 32 %) exhibited acceptable drug release (94 to 99 %) profile but having comparatively shorter shelf life in comparison to optimized K4M9 formulation. Excessive retardation in drug release was observed in valsartan CR formulations containing blend of Methocel® K4M & Kollidon® SR at various concentrations. Drug release kinetics of valsartan controlled release tablets were analyzed in various dissolution media using different mathematical models like first order, zero order, Hixon-Crowell, Higuchi, Weibull, Bakers-Lonsdale and Korsmeyer designs. DDSolver® Microsoft Excel based software was used to calculate the regression coefficients and release constants. Among all Methocel® valsartan controlled release formulations, K4M9 indicated higher linearity values for zero order, Korsmeyer-Peppas and Weibull kinetics at pH 1.2, 4.5 & 6.8. Non Fickian or anomalous diffusion release (n > 0.45) was observed showing erosion and diffusion of drug in controlled manner. β value of Weibull model was greater than 1, presenting sigmoid curve which indicated initial slower release followed by a rapid drug liberation. K4M2, K4M3 & KSR2 trial formulations exhibited higher similarity factor (f2) against K4M9 formulation, which was taken as reference due to the best physicochemical characteristics and controlled release profile. Response surface methodology was utilized to demonstrate the effect of independent variables (Polymer and Avicel PH 101 concentrations) on the responses (release of drug at 2, 8 and 16 h). Quadratic model analysis and P-value of coefficients showed strong influence of polymer on responses as compared to Avicel PH 101. Stability of controlled release formulations (K4M2, K4M3, K4M9, E7FP3, E7FP9, KSR2, KSR9 and K4M : KSR11) with desired drug release profiles were evaluated as per ICH guidelines. Samples were analyzed at long term (25±2 oC / 60±5 % RH) and accelerated (40±2 °C / 75±5 % RH) conditions. Swelling behavior of formulations containing Kollidon® SR and Methocel® K4M was also assessed. Results showed Methocel® polymer had the highest hydration ability as compared to Kollidon® SR. Methocel® and Kollidon® SR based valsartan formulations presented variable buoyancy times (< 15 h) without using any gas generating ingredients. With reference to buoyancy values, HPMC (K4M) polymers containing formulations displayed good floating lag time. Formulation K4M9 was selected as the most optimized formulation on the basis of physicochemical characteristics, desired drug release profile and zero order release kinetics among all the other formulations. Reproducibility of the complete adopted methodology was analyzed by preparing three separate lots of the optimized formulation K4M9. In vitro testing was repeated in all dissolution media and the f2 values confirmed the robustness and reproducibility of the developed formulation. A modified and validated HPLC technique was employed for the assessment of valsartan in human plasma. HPLC (LC-20A, Shimadzu, Kyoto, Japan) consisting of auto-sampler SIL-20A, column oven CTO-20A and PDA detector SPDM-20A equipped with Zorbax SB-C18 column (5 μm, 4.6 mm × 15 cm) adjusted at 40 °C was used to obtain chromatographic separation. LC solution software was used for chromatogram generation and data analysis. Mobile phase containing acetonitrile, water and glacial acetic acid in the ratio of 40 : 59 : 1 (pH 2.9) was pumped to the column with a flow rate of 1 mL/min. Each sample of valsartan was eluted at 4.1±0.2 min with a total run time of 8 min. Assay of valsartan was performed after extraction of drug with acetonitrile from plasma using precipitation method. In vivo pharmacokinetics and bioavailability studies of optimized (K4M9) controlled release valsartan tablet (160 mg) against reference immediate release (IR) brand (Diovan®) of same dose were carried out in local healthy subjects. Comparative bioavailability study of valsartan controlled release tablet with immediate release tablets was performed due to unavailability of controlled release brand in commercial market. Following FDA guidelines a single dose, open label, two treatments, two period, cross over pharmacokinetic study was conducted, comprising of twelve healthy young male Compartmental and non-compartmental parameters of valsartan controlled release formulations were computed by Kinetica® (version 5.1) software. Significant difference (P < 0.05) was observed between pharmacokinetics of test and reference tablets. The Cmax and Tmax of the commercial brand and the trial product (K4M9) were found to be 3.062±0.008 μg/mL, 2.396±0.016 μg/mL and 2.597±0.013 h, 5.844±0.027 h respectively. Considerable change in AUC0-t was also observed between reference (23.668±0.330 μg/mL.h) and K4M9 (50.723±0.414 μg/mL.h). The mean residence time of the currently developed formulation was found to be two folds greater than the reference IR tablets. Similarly, the T1/2Kel values of reference immediate release (Diovan®) vs. test controlled release (K4M9) were estimated as 6.023±0.473 h and 11.188±0.720 h respectively. This work focused on the designing of a quality pharmaceutical product with simple, cost effective methodology that could be beneficial for pharmaceutical industries. The findings of the current study will be helpful in the development of the controlled release valsartan tablets by direct compression method using different polymers. The pharmacokinetic evaluation of the newly designed formulation in healthy human subjects assured the steady drug plasma profile in biological system. Therefore, valsartan CR tablets will overcome the drawbacks associated with the conventional immediate release therapy resulting in better patient compliance and drug adherence." xml:lang="en_US