Your search keyword '"Imteyaz Qamar"' showing total 38 results

1. Ligand based-design of potential schistosomiasis inhibitors through QSAR, homology modeling, molecular dynamics, pharmacokinetics, and DFT studies

Author

Saudatu C. Ja'afaru, MChem, Adamu Uzairu, PhD, Anshuman Chandra, PhD, Muhammed S. Sallau, PhD, George I. Ndukwe, PhD, Muhammad T. Ibrahim, PhD, and Imteyaz Qamar, PhD

Subjects

Glutathione S-transferase, Ligand based drug design, Molecular docking simulations, Schistosoma mansoni, Schistosomiasis, Medicine (General), R5-920

Abstract

الملخص: أهداف البحث: داء البلهارسيات هو مرض استوائي مهمل وسبب رئيسي للوفيات في المناطق المتضررة. في الوقت الحاضر، لا يوجد لقاح عملي لمكافحة داء البلهارسيات، مما يضع الاعتماد الكبير على الاستخدام الواسع النطاق لعقار البرازيكوانتيل. يثير الاستخدام الشامل لعقار برازيكوانتيل مخاوف بشأن ظهور المقاومة للأدوية. ونتيجة لذلك، هناك حاجة إلى أهداف علاجية جديدة ومركبات محتملة لمكافحة داء البلهارسيات. طريقة البحث: تم تحسين أربعة وعشرين مشتقا قويا من البرازيكوانتيل من خلال نظرية الكثافة الوظيفية عند مستوى ''ب3ليب/6-31ج''. تم إنشاء نماذج العلاقة الكمية بين الهيكل والنشاط، وتم التحقق من صحتها إحصائيا وتم اختيار المرشح الرئيسي بهدف تطوير المزيد من الخيارات العلاجية مع تحسين الفعالية تجاه داء البلهارسيات. تم تقييم الطاقات البيولوجية وطاقة الارتباط للمركبات المصممة. كما تم إجراء دراسات الديناميكية الجزيئية والتشابه الدوائي والامتصاص والتوزيع والتمثيل الغذائي والإفراز والسمية والكثافة الوظيفية على المركبات المصممة حديثا. النتائج: تم إنشاء خمسة نماذج لعلاقة الهيكل بالنشاط الكمي، من بينها تفوق النموذج 1 بمعلمات التحقق المفضلة، وتم اختياره لتحديد مرشح رئيسي. المعلمات الإحصائية الأخرى للنموذج المختار كانت تتراوح قيم عامل تضخم التباين من 1.242 إلى 1.678 ومعامل التخليط البالغ 0.747. تم تصميم خمسة مركبات جديدة أظهرت أنشطة متوقعة محسنة (تتراوح من 5.081 إلى 7.022)، متجاوزة كلا من الرصاص والبرازيكوانتيل المتوقع البالغ 5.545 .يكشف تحليل محاكاة الديناميكيات الجزيئية عن تقارب الارتباط العالي للمركبات المقترحة تجاه المستقبل المستهدف. تظهر تقييمات الامتصاص والتوزيع والتمثيل الغذائي والإفراز والسمية والتشابه مع الأدوية الالتزام بمعايير ليبينسكي، مما يشير إلى السلامة الدوائية والفموية. كما يشير تحليل نظرية الكثافة الوظيفية إلى مقاومة التغير الإلكتروني أثناء التفاعلات الكيميائية. الاستنتاجات: تظهر المركبات المقترحة خصائص الأدوية المحتملة، مما يشير إلى مدى ملاءمتها لمزيد من البحث لتعزيز خيارات علاج داء البلهارسيات. Abstract: Objectives: Schistosomiasis, a neglected tropical disease, is a leading cause of mortality in affected geographic areas. Currently, because no vaccine for schistosomiasis is available, control measures rely on widespread administration of the drug praziquantel (PZQ). The mass administration of PZQ has prompted concerns regarding the emergence of drug resistance. Therefore, new therapeutic targets and potential compounds are necessary to combat schistosomiasis. Methods: Twenty-four potent derivatives of PZQ were optimized via density functional theory (DFT) at the B3LYP/6-31G∗ level. Quantitative structureactivity relationship (QSAR) models were generated and statistically validated, and a lead candidate was selected to develop therapeutic options with improved efficacy against schistosomiasis. The biological and binding energies of the designed compounds were evaluated. In addition, molecular dynamics; drug-likeness; absorption, distribution, metabolism, excretion, and toxicity (ADMET); and DFT studies were performed on the newly designed compounds. Results: Five QSAR models were generated, among which model 1 had favorable validation parameters (R2train: 0.957, R2adj: 0.941, LOF: 0.101, Q2cv: 0.906, and R2test: 0.783) and was chosen to identify a lead candidate. Other statistical parameters for the chosen model included variance inflation factor values ranging from 1.242 to 1.678, and a Y-scrambling coefficient (cRp2) of 0.747. Five new compounds were designed with improved predicted activity (ranging from 5.081 to 7.022) surpassing those of both the lead compound and PZQ (predicted pEC50 of 5.545). Molecular dynamics simulation revealed high binding affinity of the proposed compounds toward the target receptor. ADMET and drug-likeness assessments indicated adherence to Lipinski's rule of five criteria, thereby suggesting pharmacological and oral safety. In addition, DFT analysis indicated resistance to electronic alteration during chemical reactions. Conclusion: The proposed compounds exhibited potential drug characteristics, thus indicating their suitability for further investigation to enhance schistosomiasis treatment options.

Published

2024

2. Revolutionizing biomedicine: Aptamer-based nanomaterials and nanodevices for therapeutic applications

Author

Rajkumari Urmi, Pallabi Banerjee, Manisha Singh, Risha Singh, Sonam Chhillar, Neha Sharma, Anshuman Chandra, Nagendra Singh, and Imteyaz Qamar

Subjects

Aptamer, Nanomaterials, SELEX, Nanodevices, Aptasensors, Nanorobots, Biotechnology, TP248.13-248.65

Abstract

With the progress in two distinct areas of nanotechnology and aptamer identification technologies, the two fields have merged to what is known as aptamer nanotechnology. Aptamers have varying properties in the biomedical field include their small size, non-toxicity, ease of manufacturing, negligible immunogenicity, ability to identify a wide range of targets, and high immobilizing capacity. Nevertheless, aptamers can utilize the distinct characteristics offered by nanomaterials like optical, magnetic, thermal, electronic properties to become more versatile and function as a novel device in diagnostics and therapeutics. This engineered aptamer conjugated nanomaterials, in turn provides a potentially new and unique properties apart from the pre-existing characteristics of aptamer and nanomaterials, where they act to offer wide array of applications in the biomedical field ranging from drug targeting, delivery of drugs, biosensing, bioimaging. This review gives comprehensive insight of the different aptamer conjugated nanomaterials and their utilization in biomedical field. Firstly, it introduces on the aptamer selection methods and roles of nanomaterials offered. Further, different conjugation strategies are explored in addition, the class of aptamer conjugated nanodevices being discussed. Typical biomedical examples and studies specifically, related to drug delivery, biosensing, bioimaging have been presented.

Published

2024

3. Repurposing of drugs against methyltransferase as potential Zika virus therapies

Author

Rohit Shukla, Anshuman Chandra, Anuj Kumar, Pallavi Kandpal, Himanshu Avashthi, Vijay Kumar Goel, Imteyaz Qamar, Nagendra Singh, David J. Kelvin, and Tiratha Raj Singh

Subjects

Medicine, Science

Abstract

Abstract In recent years, the outbreak of infectious disease caused by Zika Virus (ZIKV) has posed a major threat to global public health, calling for the development of therapeutics to treat ZIKV disease. Several possible druggable targets involved in virus replication have been identified. In search of additional potential inhibitors, we screened 2895 FDA-approved compounds using Non-Structural Protein 5 (NS5) as a target utilizing virtual screening of in-silco methods. The top 28 compounds with the threshold of binding energy −7.2 kcal/mol value were selected and were cross-docked on the three-dimensional structure of NS5 using AutoDock Tools. Of the 2895 compounds screened, five compounds (Ceforanide, Squanavir, Amcinonide, Cefpiramide, and Olmesartan_Medoxomil) ranked highest based on filtering of having the least negative interactions with the NS5 and were selected for Molecular Dynamic Simulations (MDS) studies. Various parameters such as RMSD, RMSF, Rg, SASA, PCA and binding free energy were calculated to validate the binding of compounds to the target, ZIKV-NS5. The binding free energy was found to be −114.53, −182.01, −168.19, −91.16, −122.56, and −150.65 kJ mol−1 for NS5-SFG, NS5-Ceforanide, NS5-Squanavir, NS5-Amcinonide, NS5-Cefpiramide, and NS5-Ol_Me complexes respectively. The binding energy calculations suggested Cefpiramide and Olmesartan_Medoxomil (Ol_Me) as the most stable compounds for binding to NS5, indicating a strong rationale for their use as lead compounds for development of ZIKV inhibitors. As these drugs have been evaluated on pharmacokinetics and pharmacodynamics parameters only, in vitro and in vivo testing and their impact on Zika viral cell culture may suggest their clinical trials on ZIKV patients.

Published

2023

4. An overview of SARS-COV-2 (COVID-19) disease pandemic

Author

Sagorika Rai, Pallabi Banerjee, Anshuman Chandra, and Imteyaz Qamar

Subjects

covid-19, epidemic, severe respiratory syndrome, pandemic, epidemiology, sars-cov-2, transmission, diagnosis, Microbiology, QR1-502

Abstract

A novel coronavirus (SARS-COV-2) overflow event, with its epicenter point in the Wuhan (China), has risen as the health of the public crisis is of global concern. This started as an episode in the December, (2019), and till the 28th of February, (2020), there have about 83,704 committed cases of the SARS-COV-2 (COVID-19) disease at the global level, including 2,859 deaths. This showed overall cases including 3.41% of the fatality rate. At this point more than 58 nations or regions were affected with SARS-COV-2 (COVID-19) disease. As an important role of the worldwide response to manage and contain this pandemic, significant accentuation was put to create research knowledge in order to manage proof based response to carry the infection. This disease was named as severe respiratory syndrome COVID-19 (SARS-CoV-2), owing to its hereditary similarities with the SARS infection. Individual to-individual transmission of the COVID-19 contamination led to the isolation of the patients that were treated with various types of treatments. Various measures have been executed to decrease the individual to-individual transmission of the SARS-CoV-2, to stop the present outbreak. Unique considerations and many efforts ought to be applied in the populations to decrease the transmission of COVID-19 including health care providers, kids and older individuals. The aims of this review were to highlight the epidemiology, transmission, diagnosis and future instructions of COVID-19 to stop spreading of this lethal disease.

Published

2020

5. Drugs swapping in coronavirus strains: a structural biology view

Author

Vaishali Gurjar, Saiyada Iqra Kamil, Anshuman Chandra, Imteyaz Qamar, and Nagendra Singh

Subjects

Structural Biology, General Medicine, Molecular Biology

Abstract

Coronavirus belongs to the coronaviridae family, having a single-stranded RNA as genetic material of 26–42 kb in size. The first coronavirus infection emerged in 2002, caused by SARS-CoV1. Since then, genome sequences and three-dimensional structures of crucial proteins and enzymes of the virus have been studied in detail. The novel coronavirus (nCoV) outbreak has caused the COVID19 pandemic, which is responsible for the deaths of millions of people worldwide. The nCoV was later renamed as SARS-CoV2. The details of most of the COV proteins are available at the atomic and molecular levels. The entire genome is made up of 12 open reading frames that code for 27 different proteins. The spike surface glycoprotein, the envelope protein, the nucleocapsid protein, and the membrane protein are the four structural proteins which are required for virus attachment, entrance, assembly, and pathogenicity. The remaining proteins encoded are called non-structural (NSPs) and support the survival of the virus. Several non-structural proteins are also validated targets for drug development against coronavirus and are being used for drug design purposes. To perform a comparative study, sequences and three-dimensional structures of four crucial viral enzymes, Mpro, PLpro, RdRp, and EndoU from SARS-CoV1 and SARS-CoV2 variants were analyzed. The key structural elements and ligands recognizing amino acid residues were found to be similar in enzymes from both strains. The significant sequences and structural resemblance also suggest that a drug developed either for SARS-CoV1 or SARS-CoV2 using these enzymes may also have the potential to cross-react. Communicated by Ramaswamy H. Sarma

Published

2023

6. Mechanistic Insights into Immunological Therapy for Targeting Diabetic Retinopathy

Author

Imteyaz Qamar

Subjects

business.industry, Medicine, Diabetic retinopathy, business, medicine.disease, Bioinformatics

Abstract

Diabetic retinopathy (DR) is a common complication amongst patients that have diabetes. It is a leading cause of blindness in middle age people. A large proportion of patients who have diabetes develop retinopathy. There are several immunological reasons associated with the pathophysiology of this disease. Role of several mediators that increase the oxidative stress and have a pro-inflammatory effect which leads to capillary occlusion and neovascularization (NV). Increased vasopermeability due to disruption of the blood-retinal barrier (BRB) leading to diabetic macular edema (DME). Immunotherapies utilise different compounds and target various inflammatory molecules like TNF-α and pathways such as PPARγ for treatment of this progressive disease. Inflammatory and pro-inflammatory pathways are found to have an essential role in promoting DR; therefore, targeting them provides a useful technique for curing DR.

Published

2021

7. In silico identification and validation of natural antiviral compounds as potential inhibitors of SARS-CoV-2 methyltransferase

Author

Meenakshi Chaudhary, Anshuman Chandra, Imteyaz Qamar, Nagendra Singh, and Vikrant Nain

Subjects

Antiviral natural compounds, Virtual screening, Methyltransferase, molecular dynamic simulation, SARS-CoV-2, Chemistry, Mechanism (biology), Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), In silico, Target analysis, General Medicine, Computational biology, MTase, Structural Biology, Docking (molecular), docking, amentoflavone, Identification (biology), Molecular Biology, Research Article

Abstract

The novel Coronavirus disease 2019 (COVID-19) is potentially fatal and caused by Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2). Due to the unavailability of any proven treatment or vaccination, the outbreak of COVID-19 is wreaking havoc worldwide. Hence, there is an urgent need for therapeutics targeting SARS-CoV-2. Since, botanicals are an important resource for several efficacious antiviral agents, natural compounds gaining significant attention for COVID-19 treatment. In the present study, methyltranferase (MTase) of the SARS-CoV-2 is targeted using computational approach. The compounds were identified using molecular docking, virtual screening and molecular dynamics simulation studies. The binding mechanism of each compound was analyzed considering the stability and energetic parameter using in silico methods. We have found four natural antiviral compounds Amentoflavone, Baicalin, Daidzin and Luteoloside as strong inhibitors of methyltranferase of SARS-CoV-2. ADMET prediction and target analysis of the selected compounds showed favorable results. MD simulation was performed for four top-scored molecules to analyze the stability, binding mechanism and energy requirements. MD simulation studies indicated energetically favorable complex formation between MTase and the selected antiviral compounds. Furthermore, the structural effects on these substitutions were analyzed using the principles of each trajectories, which validated the interaction studies. Our analysis suggests that there is a very high probability that these compounds may have a good potential to inhibit Methyltransferase (MTase) of SARS-CoV-2 and to be used in the treatment of COVID-19. Further studies on these natural compounds may offer a quick therapeutic choice to treat COVID-19. Communicated by Ramaswamy H. Sarma

Published

2021

8. Identification of a novel and potent small molecule inhibitor of SRPK1: mechanism of dual inhibition of SRPK1 for the inhibition of cancer progression

Author

Imteyaz Qamar, Nagendra Singh, Anshuman Chandra, and Hanumappa Ananda

Subjects

Aging, flow cytometery, Cell Survival, Apoptosis, Protein Serine-Threonine Kinases, SRPK1, environment and public health, Serine, Inhibitory Concentration 50, Jurkat Cells, Humans, RNA, Messenger, Phosphorylation, Binding site, Protein kinase A, Protein Kinase Inhibitors, Cell Proliferation, chemistry.chemical_classification, MTT assay, Cell Death, Serine-Arginine Splicing Factors, Kinase, splicing inhibitor, Cell Biology, virtual screening, Small molecule, Cell biology, Molecular Docking Simulation, Enzyme, chemistry, A549 Cells, structure based drug design, Drug Design, Drug Screening Assays, Antitumor, K562 Cells, Research Paper, HeLa Cells

Abstract

Protein kinases are the family of attractive enzyme targets for drug design with relevance to cancer biology. Serine arginine protein kinase 1 (SRPK1) is responsible for the phosphorylation of serine/arginine (SR)-rich proteins. Alternative Splicing Factor/Splicing Factor 2 (ASF/SF2) involved in mRNA editing. ASF/SF2 is over expressed in many cancers and plays crucial roles in the cell survival. Phosphorylation of ASF/SF2 is decisive for its functions in cancer. In search of potential anticancer therapeutic agents for attenuating phosphorylation of ASF/SF2, we have explored specific and potential inhibitors of SRPK1 from natural and drug like compounds databases using in-silico methods. Compound ZINC02154892 (C02) was found to be the most potent inhibitor for SRPK1. In-vitro molecular and cell biology studies have shown C02 as a potent and specific inhibitor of phosphorylation of ASF/SF2 and cell survival in leukemic cell line. Structural analysis of SRPK1 with compound C02 revealed a unique pattern of binding targeting ATP binding site along with inhibiting recruitment of ASF/SF2 by SRPK1. The possibilities of compound C02 to be used as a lead compound paving way for the development of potent and specific inhibitors of SRPK1 for designing of novel potential anticancer inhibitor is inferred from the current studies.

Published

2020

9. Author response for 'Prognostic utility of key copy number alterations in T cell acute lymphoblastic leukemia'

Author

null Sarita Kumari, null Md Shadab Ali, null Jay Singh, null Mohit Arora, null Deepak Verma, null Avanish Kumar Pandey, null Mercilena Benjamin, null Sameer Bakhshi, null Jayanth Kumar Palanichamy, null Atul Sharma, null Inder Singh, null Pranay Tanwar, null Amar Ranjan Singh, null Deepam Pushpam, null Imteyaz Qamar, and null Anita Chopra

Published

2022

10. Prognostic utility of key copy number alterations in T cell acute lymphoblastic leukemia

Author

Sarita Kumari, M. Shadab Ali, Jay Singh, Mohit Arora, Deepak Verma, Avanish Kumar Pandey, Mercilena Benjamin, Sameer Bakhshi, Jayanth Kumar Palanichamy, Atul Sharma, Inder Singh, Pranay Tanwar, Amar Ranjan Singh, Deepam Pushpam, Imteyaz Qamar, and Anita Chopra

Subjects

Adult, Cancer Research, Protein Tyrosine Phosphatase, Non-Receptor Type 2, Oncology, DNA Copy Number Variations, Mutation, Humans, Hematology, General Medicine, Child, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma, Prognosis

Abstract

T-cell acute lymphoblastic leukemia (T-ALL) is a genetically heterogeneous disease, characterized by an abnormal transformation of T cells into highly proliferative leukemic lymphoblasts. Identification of common genetic alterations has provided promising opportunities for better risk stratification in T-ALL. Current treatment in T-ALL still poses the major challenge of integrating the knowledge of molecular alterations in the clinical setting. We utilized the Multiplex Ligation Dependent Probe Amplification (MLPA) method to determine the frequency of common copy number alterations (CNAs) in 128 newly diagnosed T-ALL patients. We also studied the association of these CNAs with patient's clinical characteristics and survival. The highest frequency of deletion was observed in CDKN2A (59.38%), followed by CDKN2B (46.88%), LMO1 (37.5%), and MTAP (28.12%). PTPN2 (22.66%), PHF6 (14.06%), and MYB (14.06%) had the highest number of duplication events. A total of 89.06% patients exhibited CNAs. STIL::TAL1, NUP214::ABL1, and LMO2::RAG2 fusions were observed in 5.47%, 3.12%, and 0.78% of patients, respectively. CDKN2A, CDKN2B, and PTPN2 gene deletions were mainly observed in pediatric patients, while CNAs of NF1 and SUZ12 were observed more frequently in adults. In pediatric patients, alterations in CDKN2B, CASP8AP2, and AHI1 were associated with poor prognosis, while SUZ12 and NF1 CNAs were associated with favorable prognosis. In adult patients, ABL1 CNA emerged as an independent indicator of poor prognosis. The observed molecular heterogeneity in T-ALL may provide the basis for variations observed in clinical response in T-ALL and MLPA based CNA detection may help in risk stratification of these patients.

Published

2022

11. An overview of SARS-COV-2 (COVID-19) disease pandemic

Author

Anshuman Chandra, Imteyaz Qamar, Pallabi Banerjee, and Sagorika Rai

Subjects

medicine.medical_specialty, Isolation (health care), Transmission (medicine), business.industry, diagnosis, pandemic, transmission, Outbreak, Disease, Microbiology, epidemic, QR1-502, sars-cov-2, covid-19, severe respiratory syndrome, Environmental health, Case fatality rate, Epidemiology, Health care, Pandemic, medicine, epidemiology, business

Abstract

A novel coronavirus (SARS-COV-2) overflow event, with its epicenter point in the Wuhan (China), has risen as the health of the public crisis is of global concern. This started as an episode in the December, (2019), and till the 28th of February, (2020), there have about 83,704 committed cases of the SARS-COV-2 (COVID-19) disease at the global level, including 2,859 deaths. This showed overall cases including 3.41% of the fatality rate. At this point more than 58 nations or regions were affected with SARS-COV-2 (COVID-19) disease. As an important role of the worldwide response to manage and contain this pandemic, significant accentuation was put to create research knowledge in order to manage proof based response to carry the infection. This disease was named as severe respiratory syndrome COVID-19 (SARS-CoV-2), owing to its hereditary similarities with the SARS infection. Individual to-individual transmission of the COVID-19 contamination led to the isolation of the patients that were treated with various types of treatments. Various measures have been executed to decrease the individual to-individual transmission of the SARS-CoV-2, to stop the present outbreak. Unique considerations and many efforts ought to be applied in the populations to decrease the transmission of COVID-19 including health care providers, kids and older individuals. The aims of this review were to highlight the epidemiology, transmission, diagnosis and future instructions of COVID-19 to stop spreading of this lethal disease.

Published

2020

12. Traditional Nutritional and Health Practices Targeting Lifestyle Behavioral Changes in Humans

Author

Mohammad Anas, Imteyaz Qamar, Aditi Singh, Pallabi Banerjee, and Nagendra Singh

Subjects

Environmental ethics, Diseases, Review Article, Traditional, medicine.disease, Lifestyle, Poliomyelitis, Health problems, Work (electrical), Health, Political science, medicine, Life expectancy, Natural (music), DIYs, Nutrition

Abstract

In this 21st century who isn't enticed by the glamorous and appealing life in the fast lane? We are surrounded by wonders, something we could never have imagined erstwhile. We have everything just a click or a call away. This alluring lifestyle comes with its own perils, the biggest one being concerned with health which is often compromised with check ins and home delivered food but the problem doesn't just lie with the outside food but also with all those chemical enriched engineered expensive food items. The industry often tempers with our food to make it "More Attractive" to the consumer. However, in modern era, availability of drugs and fancy powders has led to imbalance of health and nutrition, contrary to the previous era when home gardening was very common and people preferred fresh-foods which didn't contain added chemicals. They even used to treat some of the health problems with the natural ways that we nowadays refer to DIYs (Do-it-yourselves). Since Ayurveda used natural herbs and plant extracts for treatment, the earth was fresher and less-polluted which led to greater life expectancy. The modern era also has its own benefits like excellences in allopathy medicine has brought a cure to many untreatable diseases of the ancient times, and have even eradicated certain diseases like smallpox and polio. To summarize, both the time had their own pros and cons, so it would be better if we take both of their advantages into consideration and work ahead to live a healthy life.

Published

2020

13. Identification of potential inhibitors of SARS-COV-2 endoribonuclease (EndoU) from FDA approved drugs: a drug repurposing approach to find therapeutics for COVID-19

Author

Anshuman Chandra, Vaishali Gurjar, Imteyaz Qamar, and Nagendra Singh

Subjects

Drug, medicine.drug_class, media_common.quotation_subject, 030303 biophysics, IC50, Pharmacology, Antiviral Agents, endonuclease, 03 medical and health sciences, chemistry.chemical_compound, Structural Biology, binding affinity, Endoribonucleases, Uridine monophosphate, medicine, Idarubicin, Humans, Molecular Biology, media_common, 0303 health sciences, Virtual screening, drug repurposing, molecular dynamic simulation, SARS-CoV-2, Drug Repositioning, COVID-19, General Medicine, Molecular Docking Simulation, Drug repositioning, chemistry, Drug development, Pharmaceutical Preparations, Antiviral drug, medicine.drug, Research Article

Abstract

SARS-CoV-2 is causative agent of COVID-19, which is responsible for severe social and economic disruption globally. Lack of vaccine or antiviral drug with clinical efficacy suggested that drug repurposing approach may provide a quick therapeutic solution to COVID-19. Nonstructural protein-15 (NSP15) encodes for an uridylate-specific endoribonuclease (EndoU) enzyme, essential for virus life cycle and an attractive target for drug development. We have performed in silico based virtual screening of FDA approved compounds targeting EndoU in search of COVID-19 drugs from commercially available approved molecules. Two drugs Glisoxepide and Idarubicin used for treatment for diabetes and leukemia, respectively, were selected as stronger binder of EndoU. Both the drugs bound to the active site of the viral endonuclease by forming attractive intermolecular interactions with catalytically essential amino acid residues, His235, His250, and Lys290. Molecular dynamics simulation studies showed stable conformation dynamics upon drugs binding to endoU. The binding free energies for Glisoxepide and Idarubicin were calculated to be –141 ± 11 and –136 ± 16 kJ/mol, respectively. The IC50 were predicted to be 9.2 µM and 30 µM for Glisoxepide and Idarubicin, respectively. Comparative structural analysis showed the stronger binding of EndoU to Glisoxepide and Idarubicin than to uridine monophosphate (UMP). Surface area calculations showed buried are of 361.8Å2 by Glisoxepide which is almost double of the area occupied by UMP suggesting stronger binding of the drug than the ribonucleotide. However, further studies on these drugs for evaluation of their clinical efficacy and dose formulations may be required, which may provide a quick therapeutic option to treat COVID-19. Communicated by Ramaswamy H. Sarma

Published

2020

14. Comprehensive review on the evolution of SARS-CoV-2(COVID-19): From emergence, outbreak,molecular characterization to the clinical challenges in designing and developing potential drugs, vaccines and therapies to counter SARSCoV-2

Author

Pallabi Banerjee, Tripti Singh, Nagendra Singh, and Imteyaz Qamar

Abstract

The outbreak of Coronavirus which initially began in China, in the year 2003 has caused several major public health concerns which resulted in epidemics globally, such as, severe acute respiratory syndrome (SARS) & Middle East respiratory syndrome (MERS). Most recently, i.e. in late December 2019, authorities identified an ongoing outbreak of the novel coronavirus (2019-nCoV), recently named as COVID-19 caused by SARS-CoV-2 which originated in Wuhan, Hubei Province, China. It probably marked the third highly pathogenic coronaviruses spreading globally, causing severe respiratory ailments and pneumonia-like infections in the humans.2019-nCoV exhibits similar genome organization, genetic, and epidemiological features to the other known CoVs. The COVID 19 virus has been declared as an inter-human transmissible virus which readily spreads mainly through the respiratory droplets produced when a person infected with coronavirus coughs, sneezes or talks. In a short stretch of time, this epidemic had spread to 210 Countries and Territories with 16, 20, 500 confirmed cases, including 97,400 confirmed deaths. Currently, the Mortality rate of COVID 19 is 2-5% only compared to SARS and MERS Coronaviruses. The older people are at a higher risk of COVID-19 infection due to their reduced immunity and body reserves, as well as multiple associated comorbidities like hypertension, diabetes, cancer and chronic obstructive pulmonary disorders. Till date, there is no effective anti-viral drug or licensed vaccine available to treat this infectious disease. As the infection is a recently advancing pathogen, several queries remain unanswered concerning the virus's reservoirs, pathogenesis, transmissibility, and much more is unknown. Herein, this article comprehensively reviews the currently available information on the virology, epidemiology, clinical presentation, diagnosis, and treatment of COVID-19.

Published

2020

15. Novel anticancer drugs related to cardiotoxicity

Author

Pallabi Banerjee and Imteyaz Qamar

Published

2022

16. Contributors

Author

Rituparna Addy, Hrushikesh Aher, Afiqah Nabihah Ahmad, Minhaz Uddin Ahmed, Ubhat Ali, Ankenapally Anjali, Aditya Arya, Neha Arya, Ashish Badiye, Pallabi Banerjee, Sudipa Bhadra, Stuti Bhagat, Sagarika Biswas, I.A. Borodina, Vikram Dalal, Hemani Dara, Vijay Kumar Garlapati, Tamás Gerecsei, O.I. Guliy, null Hemansi, Robert Horvath, Neeti Kapoor, Manoj Kumar, Sándor Kurunczi, Chitra Padmakumari Kurup, Wei Juen Liew, Syazana Abdullah Lim, Mukund Mali, Pawan Kumar Maurya, Georgia-Paraskevi Nikoleli, PrafullaKumar Patil, Beatrix Péter, Imteyaz Qamar, Mohammad Rizwan, Roslynna Rosli, Siti Noorfatimah Safar, Bichismita Sahu, Jitendra Kumar Saini, Surajbhan Sevda, Juhi Shah, Nimit Shah, Ritesh K. Shukla, Sanjay Singh, Bálint Szabó, Inna Székács, Rita Ungai-Salánki, Ankit Yadav, Somu Yadav, and B.D. Zaitsev

Published

2022

17. Cardiovascular toxicity and therapeutic modalities targeting cardio-oncology

Author

Imteyaz Qamar

Published

2022

18. Contributors

Author

Rizwan Ahmad, Yasmin Ahmad, Haseeb Ahsan, Wahid Ali, Alexander Bambokian, Elisa Brietzke, null Deepika, Archna Dhasmana, Fabiano A. Gomes, Mohammad Yusuf Hasan, Medha Kaushik, Pooja Kaushik, Akshay Kumar, Sumira Malik, Pawan Kumar Maurya, Roumen Milev, Swaraj Mohanty, Suhel Parvez, Shilpa Prasad, Imteyaz Qamar, Vikas Saini, Priyanka Sharma, Calvin Sjaarda, Claudio N. Soares, Neha Srivastava, null Uditi, Mari Uyeda, and Somu Yadav

Published

2022

19. Insights into the technological and nutritional aspects of lactic milk drinks: buttermilk

Author

Pallabi Banerjee and Imteyaz Qamar

Published

2022

20. Novel Therapeutic Approaches Targeting Oxidative Stress

Author

Imteyaz Qamar

Published

2022

21. Critical insights into cardiotoxicity of anthracyclines

Author

Hanumappa Ananda and Imteyaz Qamar

Published

2022

22. List of contributors

Author

Muhammad Aamir, Muhammad Afzaal, Aftab Ahmed, Faqir Muhammad Anjum, Huda Ateeq, Chinaza Godswill Awuchi, Muhammad Azam, Pallabi Banerjee, Pradip V. Behare, Kshirod Behera, Adnan A. Bekhit, Sourish Bhattacharya, H. Ceren Akal, Priyanka Choudhury, Adriano Gomes da Cruz, Praveen Dahiya, M. Deepa, Disney Ribeiro Dias, Kusum Dua, Kashyap Kumar Dubey, Adriana Torres Silva e Alves, Erick Almeida Esmerino, Sukanta Ghosh, Srilekha GKP, Luna Goswami, Maria Gullo, Sushma Gurumayum, Basavaprabhu Haranahalli Nataraj, Ali Ikram, Surender Jangra, Shipra Jha, Arun Karnwal, Pardeep Kaur, Sawinder Kaur, Sonali Kesarwani, Devendra Kumar, Punit Kumar, Rajeev Kumar, Jaya Lakkakula, Karina Teixeira Magalhães-Guedes, Nomvano Mketo, Sonia Morya, Ravinder Nagpal, Harshita Naithani, Juan Napoles, Arno Neumann, Muhammad Nouman, Sebnem Ozturkoglu-Budak, Sandeep Kumar Panda, Kapil Parihar, Tatiana Colombo Pimentel, T. Poongodi Vijayakumar, Imteyaz Qamar, Tilak Raj, Prasad Rasane, Brigitte M. Richard, Manikant Roy, Rohan Samir Kumar Sachan, Farhan Saeed, Muhammad Saeed, Sradhanjali Sahu, Heba H. Salama, Shallu Samyal, Sardul Singh Sandhu, A. Sankaranarayanan, Mahipal Singh Sankhla, Rosane Freitas Schwan, Mridul Shakya, Ankur Sharma, Urjita Sheth, Márcia Cristina Silva, Jyoti Singh, Swaroop S Sonone, Leila Maria Spadoti, Ramalingam Srinivasan, null Sujata, Himja Tiwari, Poonam Verma, Rohit Kumar Verma, Ashish Vyas, Pallavi Vyas, Abdulhadi Yakubu, Iqra Yasmin, Patricia Blumer Zacarchenco, and Teresa Zotta

Published

2022

23. Nanobiomaterials in biomedicine: Designing approaches and critical concepts

Author

Pallabi Banerjee and Imteyaz Qamar

Published

2022

24. High SPAG5 Expression Is Associated With Oncological Features in Endometrial Carcinoma

Author

Imteyaz Qamar, Anita Chopra, Jay Singh, Jayanth Kumar Palanichamy, Sarita Kumari, Shyam S. Chauhan, and Mohit Arora

Subjects

Expression (architecture), business.industry, Carcinoma, Cancer research, Medicine, business, medicine.disease

Abstract

Sperm-associated Antigen 5 (SPAG5, also called astrin) is a mitotic spindle protein. SPAG5 has emerged as a promising biomarker and therapeutic target in a variety of cancers. However, its expression and role in endometrial cancer (EC) remain to be studied. Using multi-omic authoritative datasets from the TCGA and CPTAC studies, we characterized theexpression, regulation of SPAG5 and its association with clinicopathological and molecular features in EC. SPAG5 was observed to be overexpressed in tumor tissues compared to controls and receiver operating characteristic analysis suggested that its mRNA levels are an excellent predictor of tumor presence (AUC>0.98). SPAG5 overexpression was associated with serous histology and The Cancer Genome Atlas (TCGA) defined molecular subtypes. Analysis of DNA methylation levels at SPAG5 genomic regions exhibiting negative correlation to SPAG5 expression. Further, SPAG5 expression was associated with copy number gain in EC. Univariate and multivariate survival analysis revealed that higher SPAG5 expression was independently associated with poor patient outcomes in EC. Additionally, gene set enrichment analysis of SPAG5 correlated genes revealed its association with numerous oncological pathways which suggest its critical involvement in this malignancy.

Published

2021

25. Structural studies on dihydrouridine synthase A (DusA) from Pseudomonas aeruginosa

Author

Nagendra Singh, Imteyaz Qamar, Nainee Goyal, and Anshuman Chandra

Subjects

Protein Folding, Circular dichroism, Flavin Mononucleotide, Stereochemistry, Equilibrium unfolding, 02 engineering and technology, Molecular Dynamics Simulation, Ligands, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, Protein Domains, RNA, Transfer, Structural Biology, Amino Acid Sequence, Molecular Biology, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, General Medicine, 021001 nanoscience & nanotechnology, Protein tertiary structure, Enzyme, chemistry, Docking (molecular), Puromycin, Pseudomonas aeruginosa, Transfer RNA, Thermodynamics, Dihydrouridine, Oxidoreductases, 0210 nano-technology

Abstract

Dihydrouridination is one of the abundant modifications in tRNA editing. The presence of dihydrouridine is attributed to tRNA stability desired for the efficient gene translation process. The conversion of uridine to dihydrouridine is catalyzed by flavine containing enzyme called dihydrouridine synthase (Dus). We report first ever information about DusA enzyme from Pseudomonas aeruginosa in form of structural and functional studies. The gene coding for DusA from P. aeruginosa (PADusA) was cloned, expressed and purified, using recombinant DNA technology methods. Thermal and chemical stability of PADusA was determined with respect to temperature and urea-induced equilibrium unfolding experiments, with monitoring the change of ellipticity at 200–260 nm by Circular Dichroism (CD) spectroscopy. Unfolding studies revealed that PADusA has acquired a stable tertiary structure fold with a Tm value of 46.2 °C and Cm of 2.7 M for urea. The enzyme contains 43% α-helices and 16% β-strands. The three dimensional structure of PADusA was modeled using insilico methods. In order to understand the mechanism of substrate recognition and catalysis, tRNA and puromycin were docked on PADusA structure and their binding was analyzed. The structural features suggested that PADusA may also form a novel target for structure based drug design of antimicrobial agents.

Published

2019

26. Exploring potential inhibitor of SARS-CoV2 replicase from FDA approved drugs using insilico drug discovery methods

Author

Anshuman Chandra, Ali S. Alqahtani, Vaishali Gurjar, Mohammad Z. Ahmed, Imteyaz Qamar, and Nagendra Singh

Subjects

Drug, In silico, media_common.quotation_subject, 030303 biophysics, RNA-dependent RNA polymerase, Pharmacology, Molecular Dynamics Simulation, Antiviral Agents, Virus, 03 medical and health sciences, Structural Biology, In vivo, Drug Discovery, Medicine, Humans, Protease Inhibitors, Molecular Biology, media_common, 0303 health sciences, Virtual screening, business.industry, Drug discovery, SARS-CoV-2, General Medicine, COVID-19 Drug Treatment, Molecular Docking Simulation, Drug repositioning, RNA, Viral, business

Abstract

Severe Acute Respiratory Syndrome Corona Virus-2 (SARS-CoV2) is responsible for fetal pneumonia called COVID19. SARS-CoV2 emerged in Wuhan, Hubei Province of China in December 2019. The COVID19 pandemic has now gripped the entire world with more than 70 million cases and over 1.5 million deaths so far. There no treatment option for COVID19 is in term of a drug or vaccine is currently available. Therefore drug repurposing may only provide a quick method for utilizing existing drugs for a therapeutic option. The virus genome contains several non-structural proteins (NSP) which serve as target for designing of antiviral agents. NSP9 of SARS-CoV2 encodes for a replicase enzyme which is essential for the virus replication in the host cell. In search of potent inhibitors, we have screened FDA approved drugs against NSP9 using in silico methods. Five drugs fluspirilene, troglitazone, alvesco, dihydroergotoxine and avodart were found to have highest affinities with the replicase. The molecular dynamics simulation (MDS) studies demonstrated strong drugs binding and stable NSP9-drugs complexes formation. The findings are also strongly supported by root-mean-square deviation, root-mean-square fluctuation, radius of gyration, and hydrogen bond analysis of the complexes. Principal component analysis showed the stable conformation of NSP9 upon drug binding. It could be inferred that these five drugs individually or in combinations may be used as potential inhibitors of NSP9 of SARS-CoV-2 after exploring their in vivo antiviral potential.Communicated by Ramaswamy H. Sarma.

Published

2021

27. Expression of Regucalcin, a calcium-binding protein is regulated by hypoxia-inducible factor-1α

Author

Tripti Singh, Pallabi Banerjee, null Uditi, Sarita Kumari, Anita Chopra, Nagendra Singh, and Imteyaz Qamar

Subjects

Male, Calcium-Binding Proteins, Intracellular Signaling Peptides and Proteins, General Medicine, Hypoxia-Inducible Factor 1, alpha Subunit, General Biochemistry, Genetics and Molecular Biology, Rats, Rats, Sprague-Dawley, A549 Cells, Animals, Humans, General Pharmacology, Toxicology and Pharmaceutics, Hypoxia, Carboxylic Ester Hydrolases

Abstract

Regucalcin (RGN) regulates intracellular Ca

Published

2022

28. Identification of hot spot residues on serine-arginine protein kinase-1 by molecular dynamics simulation studies

Author

Imteyaz Qamar, Anshuman Chandra, Nagendra Singh, and Nainee Goyal

Subjects

viruses, Molecular Dynamics Simulation, Protein Serine-Threonine Kinases, SRPK1, Arginine, environment and public health, Serine, Molecular dynamics, Splicing factor, chemistry.chemical_compound, Structural Biology, Phosphorylation, Protein kinase A, Molecular Biology, Dipeptide, Serine-Arginine Splicing Factors, Chemistry, Nuclear Proteins, RNA-Binding Proteins, Substrate (chemistry), virus diseases, Arginine Kinase, General Medicine, Biophysics, Protein Kinases

Abstract

Serine-arginine protein kinase-1 (SRPK1) is a highly specific kinase that recognizes serine-arginine dipeptide repeats and phosphorylates SR rich splicing factor ASF/SF2 in a cell-cycle regulated manner. SRPK1 processively phosphorylates serine residues on its substrate ASF/SF2. Elevated expression pattern of both SRPK1 and ASF/SF2 and their association with various carcinomas have established SRPK1 as a potent target for drug design against cancers. In order to develop specific inhibitors the binding of ASF/SF2 to SRPK1 is desired to be selectively interrupted. We have performed molecular dynamics simulation studies on crystal structure of SRPK1 complex with ASF/SF2. The ASF/SF2 acquired a stable binding on the surface of SRPK1 with strong attractive forces. Analysis revealed that there was no major position shifting of the core β-sheet region within the catalytic site of SRPK1 when present in the state of ASF/SF2 bound in comparison to apo form. Global motions of SRPK1 indicated that major stable structural changes occurred after the substrate binding. The interactions between SRPK1 and ASF/SF2 were examined and calculated during molecular dynamics simulation of 1 µs. Molecular dynamics study indicated Arg84, Lys85, Leu86, Lys174, Tyr227 and Leu479 residues of SRPK1 as essential hot spots involved in the stable binding with substrate. Structural analysis of the binding affinity and hot spot investigation provided significant information on ASF/SF2 binding which may also be considered for designing of the novel specific inhibitors of SRPK1 for the applications in cancer therapy.Communicated by Ramaswamy H. Sarma.

Published

2020

29. Novel Therapeutic Approaches Targeting Oxidative Stress

Author

Pawan Kumar Maurya, Imteyaz Qamar, Pawan Kumar Maurya, and Imteyaz Qamar

Abstract

Novel Therapeutic Approaches Targeting Oxidative Stress investigates the role of oxidative stress in disease and explores the latest methods and approaches to targeting oxidative stress for treatment and diagnosis. The book begins with an introduction to oxidative stress and its significance. Subsequent sections cover biochemical methods for detecting free radicals and novel therapeutic approaches for targeting oxidative stress in a number of different diseases. This includes age-related illnesses, neuropsychiatric disorders such as schizophrenia and bipolar disorder, and neurodegenerative diseases like Alzheimer's and Parkinson's disease. Novel approaches for targeting oxidative stress in cancer and cardiovascular diseases are also explored. The book then moves on to discuss advances in drug delivery systems and detecting oxidative stress biomarkers using biosensors. It concludes with case studies that illustrate the targeting of oxidative stress and future perspectives. - Explores oxidative stress in a variety of diseases, including neurological disorders, cardiovascular diseases, age-related diseases, and cancer - Covers a range of therapeutic approaches to target oxidative stress - Includes chapters on the application of novel drug delivery systems and diagnostic biosensors to oxidative stress - Features case studies illustrating the targeting of oxidative stress

Published

2022

30. Cardiovascular Toxicity and Therapeutic Modalities Targeting Cardio-oncology : From Basic Research to Advanced Study

Author

Imteyaz Qamar, Pawan Kumar Maurya, Imteyaz Qamar, and Pawan Kumar Maurya

Abstract

Cardiovascular Toxicity and Therapeutic Modalities Targeting Cardio-Oncology: From Basic Research to Advanced Study analyzes the emerging the field of cardio-oncology, reviewing recent advancements in the field, discussing how to monitor and treat cancer survivors for cardiotoxicity, and identifying potential cardiac side effects in novel cancer therapies. By adopting a translational approach, the book first comprehensively covers the basic science, mechanisms and concepts, which is followed by advanced state-of-art of cardio-oncology. Other sections cover tyrosine kinase inhibitors, Anthracyclines, and biomarkers in cardiotoxicity induced by chemotherapeutic drugs, noninvasive cardiovascular imaging techniques, radiotherapy induced cardiovascular, and more. Anti-cancer treatment is associated with serious cardiovascular adverse events, including arterial and pulmonary hypertension, supraventricular and ventricular arrhythmias, systolic and diastolic cardiac dysfunction and coronary artery disease. Progress in cancer therapy over the past decades improved long-term survival but increased cancer therapy-related cardiotoxicity. Both traditional chemotherapeutic agents and newer therapies have demonstrated profound cardiovascular toxicities. It is important to understand the mechanisms of these toxicities to establish strategies for the prevention and management of complications—arrhythmias, heart failure, and even death. - Adopts a translational approach and comprehensively covers the basic science, mechanisms and concepts of cardio-oncology - Outlines the current knowledge of biomarkers in cancer therapy-related cardiotoxicity - Provides an understanding of the mechanisms of cardiovascular toxicity of various therapies that may lead to the identification of novel targets to reduce vascular complications

Published

2022

31. Molecular associations and clinical significance of core NHEJ pathway genes in renal clear cell carcinoma

Author

Deepak Verma, Shyam S. Chauhan, Anita Chopra, Mohit Arora, Jay Singh, Jayanth Kumar Palanichamy, Sarita Kumari, and Imteyaz Qamar

Subjects

0301 basic medicine, Mutation, DNA Repair Pathway, DNA repair protein XRCC4, Biology, LIG4, medicine.disease_cause, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, chemistry, 030220 oncology & carcinogenesis, DNA methylation, Gene expression, Genetics, Cancer research, medicine, Gene, DNA

Abstract

Non-homologous End Joining (NHEJ) DNA damage repair pathway is the predominant pathway of DNA double-strand repair in human cells and its aberrant activity is associated with drug resistance in multiple cancers. However, the role of the NHEJ pathway in clear cell type of renal cell carcinoma (ccRCC) has been rarely addressed. We utilized authoritative databases of ccRCC containing multi-omics data, such as mutation, gene expression, DNA methylation, copy number alterations, and high throughput protein estimations to determine alterations in seven core NHEJ genes, including XRCC4, XRCC5, XRCC6, PRKDC, LIG4, NHEJ1, and PAXX. We further determined the association of their expression with clinicopathological features and molecular alterations in ccRCC. A comprehensive analysis of these genes revealed several alterations in the expression of these genes. Interestingly, NHEJ1 is downregulated and associated with better prognosis while PAXX is upregulated in ccRCC and associated with poor prognosis. These results suggest that alterations in DNA repair pathway are common in ccRCC and may provide novel therapeutic opportunities for this malignancy.

Published

2021

32. Nonsteroidal Anti‐Inflammatory Drugs ( <scp>NSAIDs</scp> )

Author

Imteyaz Qamar, Sanjit Kumar, and Nagendra Singh

Subjects

Nonsteroidal, biology, business.industry, medicine.drug_class, Inflammation, Pharmacology, Anti-inflammatory, chemistry.chemical_compound, chemistry, medicine, biology.protein, Cyclooxygenase, medicine.symptom, business

Published

2017

33. Novel PARP inhibitors sensitize human leukemic cells in an endogenous PARP activity dependent manner

Author

Mahesh Hegde, Imteyaz Qamar, Chottanahalli S. Pavankumar, Kempegowda Mantelingu, Hassan A. Swarup, Kanchugarakoppal S. Rangappa, and Sathees C. Raghavan

Subjects

0301 basic medicine, DNA repair, DNA damage, Cell growth, General Chemical Engineering, Poly ADP ribose polymerase, General Chemistry, Molecular biology, Biochemistry, Olaparib, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, PARP1, chemistry, Cancer cell, PARP inhibitor, Cancer research

Abstract

Poly(ADP-ribose) polymerase (PARP) is a critical nuclear enzyme which safeguards genome stability from genotoxic insults and helps in DNA repair. Inhibition of PARP results in sustained DNA damage in cancer cells. PARP inhibitors are known to play an important role in chemotherapy as single agents in many DNA repair pathway deficient tumor cells or in combination with several other chemotherapeutic agents. In the present study, we synthesize and characterize novel pyridazine derivatives, and evaluate their potential for use as PARP inhibitors. Results show that pyridazine derivatives inhibited the PARP1 enzymatic activity at the nanomolar range and showed anti-proliferative activity in leukemic cells. Interestingly, human leukemic cell line, Nalm6, in which PARP1 and PARP2 expression as well as intrinsic PARP activity are high, showed significant sensitivity for the novel inhibitors compared to other leukemic cells. Among the inhibitors, P10 showed maximum inhibition of intrinsic PARP activity and inhibited cell proliferation in Nalm6 cells. Besides P10 also showed maximum inhibition against purified PARP1 protein, which was comparable to olaparib in our assays. Newly synthesized compounds also showed remarkable DNA trapping ability, which is a signature feature of many PARP inhibitors. Importantly, P10 also induced late S and G2/M arrest in Nalm6 cells, indicating accumulation of DNA damage. Therefore, we identify P10 as a potential PARP inhibitor, which can be developed as a chemotherapeutic agent.

Published

2016

34. Involvement of Calcium and Vitamin C in Type 2 Diabetes

Author

Imteyaz Qamar, Siddharth Priyadarshi, and Anubha Shukla

Subjects

Calcium metabolism, medicine.medical_specialty, Diabetes risk, business.industry, chemistry.chemical_element, Type 2 diabetes, Calcium, medicine.disease, Obesity, High cholesterol, Endocrinology, chemistry, Weight loss, Diabetes mellitus, Internal medicine, medicine, medicine.symptom, business

Abstract

The diabetes type 2 or diabetes mellitus (type 2DM) is an increasing at a frightening rate both national level and worldwide, with more than 3 million new cases per year diagnosed in the United States alone. Diabetes is the third leading cause of death in the United States, and it is also a major cause of significant morbidity. Although our current methods of treating type 2 DM and its complications have improved, prevention of the disease is preferable. Indeed, epidemiology suggest that 4 out of 5 cases of type 2 DM could be attributed to habits and forms of the modifiable behavior like obesity, sedentary lifestyle, unhealthy eating habits, family history and genetics, high blood pressure and high cholesterol. Although weight loss has been shown to be successful in delaying diabetes type 2, it is difficult to achieve and maintain for long term. Therefore, identification of environmental and easily modified risk factors is needed to prevent development of diabetes type 2. The major and most well-known function of vitamin C is to maintain calcium and potassium homeostasis and promote bone mineralization. However, recent evidence suggests that vitamin C and calcium homeostasis may also be important for a variety of non-skeletal outcomes and provide neutralizing oxygen free radicals in the body. Based on basic studies, vitamin C and calcium have also been suspected as modifiers of diabetes risk. More recently, there is accumulating evidence to suggest that altered vitamin C and calcium homeostasis may also play a role in the growth of diabetes type 2. The purpose of our systematic review was to examine: 1) the association between vitamin C & calcium status and risk of diabetes type 2. 2) The effect of vitamin C and calcium supplementation on glucose metabolism 1

Published

2012

35. A time-course study of long term over-expression of ARR19 in mice

Author

Mohammad Faiz Ahmad, Arul Narayanasamy, and Imteyaz Qamar

Subjects

Male, medicine.medical_specialty, Cellular differentiation, Biology, medicine.disease_cause, Article, Histone Deacetylases, Adenoviridae, Andrology, Mice, Prostate, Internal medicine, Testis, medicine, Animals, Humans, Testosterone, Progesterone, Epididymis, Multidisciplinary, Sexual differentiation, MARVEL Domain-Containing Proteins, Gene Expression Regulation, Developmental, Cell Differentiation, HDAC4, Androgen receptor, Repressor Proteins, medicine.anatomical_structure, Endocrinology, Receptors, Androgen

Abstract

A leucine-rich protein, ARR19 (androgen receptor corepressor-19 kDa), is highly expressed in male reproductive organs and moderately in others. Previously, we have reported that ARR19 is differentially expressed in adult Leydig cells during the testis development and inhibits steroidogenesis by reducing the expression of steroidogenic enzymes. Whereas in prostate, ARR19 represses the transcriptional activity of AR (androgen receptor), it is important for male sexual differentiation and maturation in prostate and epididymis, through the recruitment of HDAC4. In this study we show that long term adenovirus mediated overexpression of ARR19 in mice testis has the potential of inhibiting the differentiation of testicular and prostatic cells by reducing the size of testis and prostate but has no effect on the growth of seminal vesicles. Further, it reduces the level of progesterone and testosterone by reducing the steroidogenic enzymes such as 3HSD, P450c17 and StAR. This is the first study reporting a time-course analysis of the implications of long term overexpression of ARR19 in mice testis and its effect on other organs such as prostate and seminal vesicles. Taken together, these results suggest that ARR19 may play an important role in the differentiation of male reproductive organs such as testis and prostate.

Published

2015

36. ARR19 (androgen receptor corepressor of 19 kDa), an antisteroidogenic factor, is regulated by GATA-1 in testicular Leydig cells

Author

Keesook Lee, Eunsook Park, Hyun Joo Lee, Eun-Yeung Gong, and Imteyaz Qamar

Subjects

Male, Transcriptional Activation, endocrine system, Mutant, Repressor, Mice, Inbred Strains, Biology, Biochemistry, Mice, Gene expression, Testis, medicine, Cyclic AMP, Animals, GATA1 Transcription Factor, Transcription, Chromatin, and Epigenetics, Binding site, Promoter Regions, Genetic, Molecular Biology, Cells, Cultured, MARVEL Domain-Containing Proteins, Leydig cell, Gene Expression Regulation, Developmental, Leydig Cells, Membrane Proteins, Cell Biology, Luteinizing Hormone, Molecular biology, Androgen receptor, Repressor Proteins, medicine.anatomical_structure, Androgens, Mutagenesis, Site-Directed, Luteinizing hormone, Corepressor

Abstract

ARR19 (androgen receptor corepressor of 19 kDa), which encodes for a leucine-rich protein, is expressed abundantly in the testis. Further analyses revealed that ARR19 was expressed in Leydig cells, and its expression was differentially regulated during Leydig cell development. Adenovirus-mediated overexpression of ARR19 in Leydig cells inhibited testicular steroidogenesis, down-regulating the expression of steroidogenic enzymes, which suggests that ARR19 is an antisteroidogenic factor. Interestingly, cAMP/luteinizing hormone attenuated ARR19 expression in a fashion similar to that of GATA-1, which was previously reported to be down-regulated by cAMP. Sequence analysis of the Arr19 promoter revealed the presence of two putative GATA-1 binding motifs. Further analyses with 5′ deletion and point mutants of putative GATA-1 binding motifs showed that these GATA-1 binding sites were critical for high promoter activity. CREB-binding protein coactivated GATA-1 and markedly increased the activity of the Arr19 promoter. Both GATA-1 and CREB-binding proteins occupied the GATA-1 motifs within the Arr19 promoter, which was repressed by cAMP treatment. Altogether, these findings demonstrate that ARR19 is the target gene of GATA-1 and suggest that ARR19 gene expression in testicular Leydig cells is regulated by luteinizing hormone/cAMP signaling via the control of GATA-1 expression, resulting in the control of testicular steroidogenesis.

Published

2009

37. Role of CYP1B1, MYOC, OPTN, and OPTC genes in adult-onset primary open-angle glaucoma: predominance of CYP1B1 mutations in Indian patients

Author

Arun, Kumar, Manjunath G, Basavaraj, Santosh K, Gupta, Imteyaz, Qamar, Abdullah Mahmood, Ali, Vineeta, Bajaj, T K, Ramesh, D Ravi, Prakash, Jyoti S, Shetty, and Syril K, Dorairaj

Subjects

genetic structures, India, Cell Cycle Proteins, Polymerase Chain Reaction, Polymorphism, Single Nucleotide, Asian People, Gene Frequency, Transcription Factor TFIIIA, Humans, Eye Proteins, Promoter Regions, Genetic, Alleles, Polymorphism, Single-Stranded Conformational, Aged, Glycoproteins, Extracellular Matrix Proteins, Polymorphism, Genetic, Genetic Variation, Membrane Transport Proteins, Middle Aged, eye diseases, body regions, Cytoskeletal Proteins, Cytochrome P-450 CYP1B1, Mutation, Proteoglycans, Aryl Hydrocarbon Hydroxylases, Glaucoma, Open-Angle, Research Article

Abstract

Purpose Mutations in the CYP1B1, MYOC, OPTN, and WDR36 genes result in glaucoma. Given its expression in the optic nerve, it is likely a mutation in the OPTC gene is also involved in initiating glaucoma. This study was designed to evaluate the involvement of the CYP1B1, MYOC, OPTN, and OPTC genes in the etiology of adult-onset primary open-angle glaucoma (POAG) found in 251 Indian patients. Methods Blood samples were obtained from individuals for DNA isolation. A combination of polymerase chain reaction-single strand conformation polymorphism, allele-specific PCR, and DNA sequencing techniques were used to detect mutations in four genes. Four microsatellite markers from the CYP1B1 candidate region and three intragenic CYP1B1 single nucleotide polymorphisms (SNPs) were used to determine the origin of the most common CYP1B1 mutations. Results Three previously known mutations (Pro193Leu, Glu229Lys, and Arg368His) and one novel (Met292Lys) mutation were found in the CYP1B1 gene. Frequencies of the most common mutations, Glu229Lys and Arg368His, in patients were 5.12% and 3.98%, respectively. The Glu229Lys and Arg368His mutations were also found in normal controls at frequencies of 5% and 2%, respectively, suggesting that these mutations might be polymorphic variants in our population. The absence of allele sharing for D2S177, D2S1346, D2S2974, and D2S2331 markers and three intragenic CYP1B1 SNPs in patients suggested multiple origins for the Glu229Lys and Arg368His variants. Two of 251 (0.8%) patients had the Gln48His mutation in MYOC. There was no difference in the frequency of a MYOC -83G>A promoter polymorphism between patients and controls. A novel OPTN mutation, Thr202Arg, was detected in one of 251 (0.4%) patients. The OPTN variant Met98Lys was detected in similar frequencies in patients and controls. No mutation was detected in OPTC. Taken together, 3.59% (9/251) of our POAG patients had mutations in the CYP1B1, MYOC, and OPTN genes. Conclusions This is the first report to document the involvement of the CYP1B1, MYOC, and OPTN genes in the etiology of POAG in the same set of Indian patients. Our study shows that mutations in these genes are rare in Indian POAG patients.

Published

2007

38. Anti-steroidogenic Factor ARR19 Inhibits Testicular Steroidogenesis through the Suppression of Nur77 Transactivation.

Author

Imteyaz Qamar, Eun-Yeung Gong, Yeawon Kim, Chin-Hee Song, Hyun Joo Lee, Sang-Young Chun, and Keesook Lee

Subjects

*PROTEINS, *ANDROGENS, *LUTEINIZING hormone, *LEYDIG cells, *TRANSCRIPTION factors, *GENE expression

Abstract

ARR19 (androgen receptor corepressor-19 kDa), a leucine-rich protein whose expression is down-regulated by luteinizing hormone and cAMP, is differentially expressed during the development of Leydig cells and inhibits testicular steroidogenesis by reducing the expression of steroidogenic enzymes. However, the molecular events behind the suppression of testicular steroidogenesis are unknown. In the present study, we demonstrate that ARR19 inhibits the transactivation of orphan nuclear receptor Nur77, which is one of the major transcription factors that regulate the expression of steroidogenic enzyme genes in Leydig cells. ARR19 physically interacts with Nur77 and suppresses Nur77-induced promoter activity of steroidogenic enzyme genes including StAR, P450c17, and 3β-HSD in Leydig cells. Transient transfection and chromatin immunoprecipitation assays revealed that ARR19-mediated reduced expression of steroidogenic enzyme genes was likely due to the interference of SRC-1 recruitment to Nur77 protein on the promoter of steroidogenic enzyme genes. These findings suggest that ARR19 acts as a novel coregulator of Nur77, in turn regulating Nur77-induced testicular steroidogenesis, and may play an important role in the development and function of testicular Leydig cells. [ABSTRACT FROM AUTHOR]

Published

2010