بسم اللہ الرحمٰن الرحیم
عصر حاضر میں قدرتی وسائل کا استحصال سنگین مسئلہ کی نوعیت اختیار کرچکا ہے۔ اقوام متحدہ کے پائیدار ترقی (Sustainable Development)کے 17 اہداف میں قدرتی وسائل کا تحفظ بھی شامل ہے۔ لیکن جدید انسان نے پائید ار ترقی(Sustainable Development) کے اصول و اہداف کو یکسر نظرانداز کردیا ہے۔اگر دیکھا جائے تو سرمایہ ومنافع کو کسی بھی جائز و ناجائز طریقے سے کمانے ، پیداوار کو تیزرفتاری سے بڑھانے کی شدید آرزو اور ذاتی خواہشات کو سماجی ودینی مفاد پر اور جلدی حاصل ہونے والے مادی فائدے کو دیرپا ترقی (Sustainable Development) پر ترجیح دینا سرمایہ دار کا شیوہ بن کر رہ گیا ہے۔ جس کی بنا پر فضا، پانی، معدنیات، حیوانات، نباتات اور زمین کی طبعی، کیمیائی اور حیاتیاتی خصوصیات میں غیر مناسب تبدیلیاں پیدا ہو تی جار ہی ہیں ۔ جس کے نتیجے میں گلوبل وارمنگ،موسمیاتی تبدیلی اور ماحولیاتی آلودگی کا مسئلہ پیداہوگیا ہے۔الغرض گلوبلائزیشن(Globalization) کے موجودہ دور میں آسائش و ترقی کی آڑ میں موجودہ انسان نے اپنے ہی ہاتھوں سے حیاتِ انسانی کو تباہی کے دہانے پر پہنچا دیا ہے۔
اللہ تعالیٰ نے انسان کو زمین کا خلیفہ بنایا اور انسان پر ذمہ داری عائد ہوتی ہے کہ زمین کا تحفظ کرے اور اس میں پائے جانے والے وسائل کا دانشمندانہ استعمال کرے تاکہ ساری انسانیت اور آئندہ نسل اس سے مستفید ہو سکے۔لیکن جدید سرمایہ دارانہ فکر کے حامل انسان نےاپنے ذاتی مفادات کی خاطر اپنے اختیارات سے تجاوز کیا اور ماحولیاتی توازن بگاڑ دیا ۔ بقول شاعر
اوزون کی چادر ہوئی چھلنی ،سو وہ میں ہوں
صنعت کی ترقی کا ہے باعث یہ حرارت
اوزون کی چادر ہوئی چھلنی ،سو وہ میں ہوں
نائب خدا کا ہوں ،مری مرضی میں جو کروں!
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The state of Bah┐walp┴r was founded in 1802 by Naw┐b Mohammad Bah┐wal Khan II. After the establishment of Pakistan the state opted to accede to the new, on 14 August 1947 October 1947. It was dominion of Pakistan, with effect from 7.1511 merged into the province of West Pakistan on 14 October Bah┐walp┴r has always been a seat of higher learning. Uch Shar┘f, a nearby ancient town, had one of the largest universities where scholars from all over the world used to come for studies. As a continuation of that tradition, J┐m‘a Abb┐siya was established in Bah┐walp┴r in the year 1925, following the academic pursuits of Jamia Al-Azhar, Egypt. The renowned scholars spread Islam by teaching Tafs┘r of Qura’n, Hadith, Fiqh, and History along with other contemporary subjects. The establishment of Jamia Abb┐sia and the arrival of religious scholars in Bah┐walp┴r bear witness that it is a scholarly and traditional state and it has been proved as a place of protection for educational, cultural and historical traditions.
Co-infection with Mycobacterium tuberculosis (M.tb), and Human immunodeficiency virus type (HIV) is a major global public health concern and a serious problem particularly in developing countries. According to the recent survey, undertaken in 2014, 1.5 million people were died due to TB, in which 0.4 million were HIV positive. Whereas, HIV’s death toll was estimated about 1.2 million. Furthermore, approximately, 9.6millionnew TB cases occurred in 2014 globally, of these12%were HIV-positive. The high rate of co-infection between M.tb and HIV makes the management of infections more challenging. The geographic and immune overlapping effects of M.tb and HIV enable themtospread and synergize the pathogenesis of both pathogens.Several studies reported that severe manifestation of TB in HIV may be due to alteration in specific cytokine production. Few lines of research have been carried out on immune pathology in context with TB and HIV infection in vivo models which investigated only small population of cytokines such as TNF α, IFN γ, IL-10, IL-6, IL-4, IL-1 , TGF β, IL-8. However, the comprehensive assessment of immune markers including cytokines, chemokines, chemokine receptors& transcription factors, etc, remain uncharacterized, particularly in thesynergic milieu of both pathogens. Therefore, the main focus of this study was to explore the early immune response developed by patients infected with M.tb, HIV alone and both (HIV/M.tb), in order to increase the understanding of the immune pathogenic mechanisms associated with both infections and to identify relevant biomarkers that contribute in modulating immune responses during HIV and M.tb infections. Additionally, the current study further sought to investigate the expression pattern of MHC class II genes (HLA-DRB1 & HLA-DQB1) in HIV/M.tb co-infected patients. For this purpose blood samples were collected from 116individuals. Out of the total, 44 were HIV mono-infected patients, 31 were M.tb mono-infected patients, 16 were co- infected HIV/M.tb patients and 25 were uninfected people without M.tb and HIV. PBMCs were isolated from each blood sample and further processed for mRNA extraction. These RNA samples were reverse transcribed into cDNA. Sequentially RT2 profiler PCR arrays, containing 70 inflammatory genes related to T-helper 1 & T-helper 2 immune subsets were performed on final set of 64 cDNA samples. According to our findings, in active Pulmonary Tuberculosis (PTB) patients who were untreated, we found significantly altered gene expression for 18 genes as compared to control.The only Interleukin (IL), that showed 3.5 folds (p<0.05) higher expression in active PTB patients was mRNA for IL-27, which is considered as a component of TH1 immune responses; however, it exhibits both; pro-inflammatory and anti-inflammatory properties. Other cytokine genes that were found to be significantly (p<0.05) downregulated include: mRNA for IL-24 (folds -2.8), mRNA for IL-7 (folds -1.5), mRNA for TGFβ(fold -1.8) & IL-2 receptor alpha (fold -1.8). Among various chemokines and chemokine receptors, the significant (p<0.05)mRNA expression pattern was obtained for CCL5 (fold -1.6) and CXCR3(folds - 7.6). The essential transcription factors for TH1/TH2 differentiation are T-bet and GATA 3 respectively.In our study, we found significant (p<0.05)downregulation of T-bet (folds- 1.7). This indicates immune dysregulation between TH1 and TH2 responses. Among other transcription mediators, the transcripts of STAT-1, which is the main inducer of IFNγ, were appeared to be significantly(p<0.05)up-regulated (folds 2.0), whereas STAT4, an essential component of the IL-12 signaling, showed diminished responses with folds -1.7 (p<0.05). In addition, mRNA for IRF1 (folds 1.3, p<0.05) and NFATC1(folds -1.4, p<0.05) were also expressed differentially in PTB patients. TH1 dysregulation is further highlighted by significant (p<0.05)down modulation of two more genes i.e. CD80 (folds -1.9) and CD28 (folds -2.5), which is involved in costimulation of T-cell activation and IL-2 secretion. These two markers (CD28 & IL-2) are also critical in maintaining T-regulatory cells and down modulation of these markers may also favor the suppression of TH1 immune responses and T- regulatory cells activity.Other mRNA that found to be significantly (p<0.05)altered, were PTGDR2, TLR-4, TYK2 and MAPK8 with folds -2.2, 1.6, -1.7&-1.3, respectively. In a nutshell, we observed active PTB patients was neither dominated by TH1, nor by TH2 signature immune responses, however, a new biomarker IL-27 was found to be a key player in TB pathogenesis and it may negatively regulate TH1 immune responses in M.tb infection. Similar analysis wasperformed on HIV patients.The differentially regulated mRNA found to be statistically significant (p<0.05)were: IL12B, STAT1, JAK2, IL-2RA, SOCS1, IL- 10, 1L-24, CTLA4, LAG3, TNFRSF9&TYK2. The transcriptional profiling among untreated HIV patients indicates two main findings, i.e. 1)TH1/TH2 antagonism:The 7.6folds higher expression of IL-12B (a potent subunit of IL-12 cytokine) along with upregulation of STAT1 (folds 2.1) and JAK2 (folds 1.4) genes, indicatesignificant inflammatory signals for TH1 immune responses. However, in contrast, higher expression of IL-10(folds 4.4), which is an anti-inflammatoryTH2 signature cytokine, and SOCS 1 (folds 2), a strong suppressive factor for TH1 immune responses, strongly counteract these pro-inflammatory responses. This suggests antagonism between TH1 and TH2 immune responses at some levels.2)T - cells dysfunction: Two folds higher expression of inhibitory receptors (CTLA4, LAG3) also indicate defects in T cell function & proliferation. Besides increased expression of inhibitory receptors, we also found abundant transcripts of TNFRSF9 (folds 2.6), which is a co-stimulatory receptor and acts contrary in order to expandT-cell clones and maintainsprotective immune responses. Therefore, combined stimulation of co-stimulatory TNFRSF9 and co-inhibitory receptorsCTLA4, LAG3, suggests dysfunctional CD4 T-cells activity. Furthermore, significant decrease in IL-2 RA(folds – 1.5, p<0.05), also reveals disrupted T-regulatory cell activity among HIV patients. Interestingly,this particular finding is common in HIV and M.tb mono-infected patients in our study. In case of HIV/M.tb co-infected patients we have noticed significant (p < 0.05) fold changes in the following genes. The up-regulated genes were LAG 3(folds 2.5), STAT1 (folds 1.7) & IRF 1(folds 1.5), whereas down-regulated genes were CCR2 (folds - 2.0), IL-4(folds -2.5), IL4R(folds -1.4), IL-24(folds -2.2), &CD40LG(folds -1.8). In the light of these observations we can interpret that co-infection of HIV and M.tbcan cause severe immune inhibition condition in same host. Up-regulation of LAG-3 (lymphocyte activation gene3), which is an immune inhibition receptor, while down regulation of CD40 LG, which playspotent role in T-cell activation and differentiation, suggest marked inhibition in immune functionality. Secondly, down regulation of CCR2, a potent chemokine receptor for several chemokines that specifically attract monocytes to the site of infection and contribute in granuloma formation, also indicates poor lymphocyte trafficking among HIV/M.tbco-infected patients. None of the cytokines was found to be significantly up-regulated. Although, the transcripts of STAT 1 & IRF 1, potent transcription factor for TH1 responses, were positively up regulated in co-infected individuals. Lastly, we investigated HLA-DRB1 & HLA-DQB1 genes expression in studied cohorts, in order to observe the genetic predispositions for HIV/M.tb co-infection. We observed no significant association of these genetic markers with co-infection, whereas, significantly higher expression of HLA-DRB1 gene (folds 3.3, p <0.05) was seen in active PTB patients only. Taking accumulated evidences together,wesuggestthatnew immune markers are playing key role in the negative modulation of host immune responses, instead of signature immune markers. Particularly, over expression of LAG-3 in HIV mono-infection and HIV/M.tb co-infections, andIL-27 in active PTB infection, were exclusive in our study. We did not find any significant contribution ofTH1/TH2 signature cytokines, mainly IFN γ,TNF α, IL-1, IL-13, IL-15,IL-3 & IL-5, whereas most fascinating outcome of this study was about IL-24(a component of IL-10 family of cytokines), the only cytokine that is found to be commonly under expressed (p<0.05) in all patient groups (TB, HIV monoinfection &their co-infection). In conclusion, this study represents potential biomarkers relevant to TB and HIV pathogenesis in Pakistani population. These biomarkers need to be further explored on different populations in order to evaluate their significance on global scale. Furthermore, the therapeutic implications of these biomarkers in HIV and M.tb infections and its associative role in other related diseases should be investigated and validated. More effective interventions and strategies would be developed against the two deadly infections only after confirmation of putative role of such molecular markers." xml:lang="en_US