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Overview of technology acceptance model and the proposed model for developing countries

Thesis Info

Author

Sobia Azeem

Supervisor

Abdul Zahid Khan

Department

Department of Technology Management

Program

MSc

Institute

International Islamic University

Institute Type

Public

City

Islamabad

Province

Islamabad

Country

Pakistan

Thesis Completing Year

2008

Thesis Completion Status

Completed

Page

208

Subject

Technology Management

Language

English

Other

MA/MSc 658.05 SOO

Added

2021-02-17 19:49:13

Modified

2023-01-06 19:20:37

ARI ID

1676721646284

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جو خانہ بدوش ہوتا ہے

جو خانہ بدوش ہوتا ہے
سنو بہلول۔۔۔!
جو خانہ بدوش ،آوارہ ، چرواہا بھی ہو۔۔۔!
وہ پرانے تبسم کو نئے موسم کی تلخیوں میں سموتا نہیں
زخموں سے بہتے گرم لہو میں۔۔۔!
خواب کی سیڑھیوں پر سبز پتے سرخ پھول سجاتے ہوئے
ایوان وفا میں دلفریب دھڑکنوں کو قتل کرتا نہیں
پرندوں کی سنتے ہوئے!
پرانی خانقاہوں کا طواف کرتے ہوئے

عزازیل کی طرح نوری فرغل اتارتا نہیں
محبتوں کا سینہ چیرتا نہیں۔۔۔چاہتوں کا جگر کھاتا نہیں

میرے بہلول۔۔۔میرے دل کے رازداں بہلول۔۔۔!
جن سے موسم گل کی آبیاری ہو۔۔۔!
وہ متاع خواب کو رقص بسمل میں ڈبوتا نہیں
ماہ کامل کا وظیفہ پڑھتے ہوئے!
تاثیر سحر کی بزم میں۔۔۔ذوق بہار کا صحیفہ پڑھتے ہوئے!
ساکنانِ شباب کو لسان جمال کے لہجے میں پکارتا ہے
اسیران درد کے زخموں کو دھوتے ہوئے!
سبز بیلوں کی جڑوں میں دل نچوڑتے ہوئے!
معصوم جذبوں کو خزانی نیزوں میں پروتا نہیں
وعدوں کے شعور میں بجتی دف سنتے ہوئے!
اہل عشق کی راہوں میں پھول بچھاتے ہوئے!
روغن چشم سے چراغ روشن کرتا ہے
عزازیل کی طرح نوری فرغل اتارتا نہیں
محبتوں کا سینہ چیرتا نہیں۔۔۔چاہتوں کا جگر کھاتا نہیں

میرے بہلول۔۔۔میرے پیارے بہلول۔۔۔!
ہم خانہ بدوشوں کا۔۔۔!
ہواؤں کے رشتے میں خوشبوؤں کو سمو کر۔۔۔!
چاندنی راتوں کی مسیحائی پر لہجہ بدلتانہیں
جو سبزہ سرخ قاصدوں کو سینے سے لگا کر۔۔۔!
نیل کی وادیوں میں۔۔۔فرات کے صحراؤں میں بکھرے صحیفوں کی تلاوت کرتا ہے
زخموں کو چھپاتے ہوئے۔۔۔پھولوں کو روندتا نہیں۔
وفا کی کہانی، دھڑکنوں کی نشانی سے!
فقیروں کے حجرے گراتا۔۔۔درویشوں کو رولاتا نہیں
عزازیل کی طرح نوری فرغل اتارتا نہیں
محبتوں کا سینہ چیرتا نہیں۔۔۔چاہتوں کا جگر کھاتا نہیں

بہلول جی۔۔۔پیارے بہلول جی۔۔۔!
جو لسان جبرائیل سے تسکین الہام کی آیتیں سنتے ہوئے!
حقیقت اسرار...

حضور انورﷺ کی رحمت کی امتیازی خصوصیات

The many aspects of the Holy Prophet’s (PBUH) personality has been defined by Allah himself in Quran many times, keeping in view the all angles of the Holy Prophet (PBUH) Character blessings for all worlds and times. The Rehmatul-il-Almeen is infinite. The Holy Prophet (PBUH) has proved such a huge chain by his character. The blessing of the Holy Prophet (PBUH) is such a supreme that, it could not be defined in such an article, but here it has been tried to throw light on some features of Holy Prophet (PBUH) blessing. As Quran says that the secret of man on the path of the Holy Prophet (PBUH). Today same way, man regardless of color, race and religious should know that the wounds of humanity could be headed by following the route of the Holy Prophet (PBUH) Sunnah. All the other ways will lead to cul-de-sac.

Prevalence, Characterization and Clinical Evaluation of Indigenous Mycobacterium Tuberculosis

A total six thousands five hundred and seventy three (6573) indigenous pulmonary and extra- pulmonary specimens were collected from tuberculosis suspicious patients of 17-67 years age group during November, 2004 to December, 200. The sputum, pus and bronchial washings were collected from five different sources, labeled and processed for initial screening. One hundred and seventy two (172) 2.616% of total (6573) tuberculosis diagnosed (AFB positive) patients were selected from six different sources. The patients were selected, regardless of their age, gender and previous therapeutic profile. The specimen comprised of 85% sputum, 10.5% puss and 4.5% bronchial washing. We considered 29.% female and 71% males with 84.% pulmonary (sputum, bronchial washing & puss) and 16% extra-pulmonary (puss & bronchial washing) specimens. Sixty six (66) resistant Mycobacterium tuberculosis strains were further studied to determine the highest level of resistance (in % age) . The clinical isolates were collected from cultured growth on Lowenstein Jensen media supplemented with antitubercular drugs at minimum inhibitory concentration (MIC) level. The parameters of study were the pattern of sensitivity/ resistance of mycobacterial TB against rifampicin, isoniazid, ethambutol and pyrazinamide, overall pattern of resistance, resistance percentages with respect of number of colonies, overall trend of resistance during Jan. - Dec. 2005, resistance pattern in percentage against five different levels (μg/ml) above their respective critical concentrations, therapeutical interpretation of drugs to evaluate the pharmacological credibility and molecular study of Pnc A gene of Mycobacterium tuberculosis responsible of resistance against pyrazinamide. The data obtained from this study showed 37 (21.5%) strains resistant and 135 (78.5%) strains sensitive to rifampicin, 25 (14.5%) strains resistant and 147 (85.5%) strains were sensitive to isoniazid, 10 (5.8%) resistant and 162 (94.2%) strains founded sensitive to Ethambutol, 47 (27.3%) resistant and 125 (72.7%) strains were founded sensitive to Pyrazinamide of total 172 clinical isolates of Mycobacterium tuberculosis. The resistance of Mycobacterium tuberculosis noted on basis of growth pattern (number of colonies) over the mycobacterial specific Lowenstein Jensen medium. Overall mono-resistance pattern was observed as 25.71% resistant to rifampicin, 8.57% resistant to isoniazid, 2.85% resistant to ethambutol and 62.85% resistant to pyrazinamide out of 20.34% mono-resistant isolates of total 172 Mycobacterium tuberculosis strains. Poly resistance profile obtained was as 19.35% Mycobacterium TB strains resistant to rifampicin & isoniazid, 22.58% resistant to isoniazid & pyrazinamide, 3.22% resistant to ethambutol & pyrazinamide, 6.45% resistant to isoniazid & pyrazinamide, 22.58% resistant to rifampicin, isoniazid and pyrazinamide, 3.22% resistant to rifampicin, ethambutol and pyrazinamide and 22.58% resistant to all of the four 1st line drugs. The resistant Mycobacterium TB having an ultimate highest level of resistance against the first line antitubercular drugs. Which were interpreted therapeutically to study the pharmacological suitability of dosage and regimen. It was observed that no any rifampicin strain inhibited at 1st and 2nd drug levels. 40.54% resistant Mycobacterium -TB strains inhibited at 3rd rifampicin level of 120ug/ml. Practically it is not feasible to maintain a plasma concentration higher than therapeutic range of 6.5±3.5ug/ml (Joel et al., 2001). It was observed that no any isoniazid strain inhibited at 1st, 2nd and 3rd drug levels. There 28% resistant Mycobacterium-TB strains inhibited at 4th isoniazid level 9ug/ml. Maximally plasma concentration that can be maintained in body is - 4ug/ml (Richard et al., 2006), therefore it can not be used in actual practice. It was observed that no any ethambutol strain inhibited at 1stand 2nd drug levels 2ug/ml and 4ug/ml. 50% resistant Mycobacterium TB strains inhibited at 3rd level of 6ug/ml. The maximum plasma concentration (Cmax) that can be maintained in tuberculosis patient during treatment protocol are described by other researchers as 3-5ug/ml (Bertram G. Katzung, 2004), 2-5ug/ml (Leon et al., 2004) and 4- 6ug/ml (Richard et al., 2006). It was observed that no any pyrazinamide resistant strain inhibited at 1st and 2nd drug levels100ug/ml and 200ug/ml. 27.66% pyrazinamide resistant Mycobacterium TB strains were inhibited at 3rd pyrazinamide level of 300ug/ml. The maximum plasma concentration than can be maintained in human body reported by different researchers are 9- 12ug/ml (Joel et al, 2001), 19ug/ml (Leon et al., 2004), 30-50ug/ml (Bertram, 2004), 37-40ug/ml (Richard et al., 2006). The genomic DNA of pyrazinamide resistant Mycobacterium TB extracted by mechanical method and examined on gel. PCR for Mycobacterium TB is specific for Mycobacterium TB complex DNA. By using the SSCP (Single Strand Conformational Polymorphism), we were able to show most divers pattern. The resistant 17.44% showed different pattern than sensitive samples. Which indicate the mutation in this domain, while 9.88% did not show any difference in mobility in comparison to sensitive samples.