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3. Design, synthesis, biological assessment and molecular modeling studies of novel imidazothiazole-thiazolidinone hybrids as potential anticancer and anti-inflammatory agents.

Author

Kamboj, Payal, Anjali, Imtiyaz, Khalid, Rizvi, Moshahid A., Nath, Virendra, Kumar, Vipin, Husain, Asif, and Amir, Mohd.

Subjects
ANTI-inflammatory agents, ANTINEOPLASTIC agents, EPIDERMAL growth factor receptors, DENATURATION of proteins
Abstract

A new series of imidazothiazole derivatives bearing thiazolidinone moiety (4a-g and 5a-d) were designed, synthesized and evaluated for potential epidermal growth factor receptor (EGFR) kinase inhibition, anticancer and anti-inflammatory activity, cardiomyopathy toxicity and hepatotoxicity. Compound 4c inhibited EGFR kinase at a concentration of 18.35 ± 1.25 µM, whereas standard drug erlotinib showed IC50 value of 06.12 ± 0.92 µM. The molecular docking, dynamics simulation and MM-GBSA binding energy calculations revealed strong interaction of compound 4c with binding site of EGFR. The synthesized compounds were evaluated for their anticancer activity by MTT assay against three human cancer cell lines A549 (Lung), MCF-7 (Breast), HCT116 (Colon), one normal human embryonic kidney cell line HEK293 and also for their EGFR kinase inhibitory activity. Few compounds of the series (4a, 4b, 4c) showed promising growth inhibition against all the tested cancer cell lines and against EGFR kinase. Among these, compound 4c was found to be most active and displayed IC50 value of 10.74 ± 0.40, 18.73 ± 0.88 against cancer cell lines A549 and MCF7 respectively whereas it showed an IC50 value of 96.38 ± 1.79 against HEK293 cell line indicating lesser cytotoxicity for healthy cell. Compounds 4a, 4b and 4c were also examined for their apoptosis inducing potential through AO/EB dual staining assay and it was observed that their antiproliferative activity against A549 cells is mediated via induction of apoptosis. Cardiomyopathy studies showed normal cardiomyocytes with no marked sign of pyknotic nucleus of compounds 4b and 4c. Hepatotoxicity studies of compounds 4b and 4c also showed normal architecture of hepatocytes. Compounds 4a-g and 5a-d were also evaluated for their in-vitro anti-inflammatory activity by protein albumin denaturation assay. Among the tested compounds 4a-d and 5a-b showed promising activity and were selected for in-vivo inflammatory activity against carrageenan rat paw edema test. Among these compounds, 4b was found to be most active in the series showing 84.94% inhibition, whereas the standard drug diclofenac sodium showed 84.57% inhibition. Compound 4b also showed low ulcerogenic potential and lipid peroxidation. Thus, compounds 4c and 4b could be a promising lead compounds for developing anticancer and anti-inflammatory agents with low toxicity and selectivity. [ABSTRACT FROM AUTHOR]

Published
2024
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6. Synthesis and biological evaluation of some novel benzoxazine-4- one and quinazolin-4-one derivatives based on anti-inflammatory commercial drugs.

Author

Khan, Shah Alam, Ahuja, Priyanka, and Husain, Asif

Subjects
BIOACTIVE compounds, ISONIAZID, QUINAZOLINONES, BENZOXAZINONES, ANTI-inflammatory agents, AMINOBENZOIC acids, BENZOXAZINES
Abstract

Benzoxazine and quinazoline are nitrogen-containing heterocyclic scaffolds found in various biologically active compounds. Due to their diverse biological actions, these heterocyclic rings serve as crucial frameworks for designing medicinal compounds. This study aimed to synthesize and assess in vivo anti-inflammatory, analgesic, and low ulcerogenic potential of a few novel benz[d][1,3]-oxazine-4-one and quinazolinone derivatives. Benzoxazinones (3a-e) were synthesized by cyclizing the carboxylic group (-COOH) of five nonsteroidal anti-inflammatory drugs viz., aceclofenac, ibuprofen, diclofenac, mefenamic acid and ketoprofen (2a-e) with anthranilic acid (1) using dry phosphorus oxychloride (POCl3 ) in pyridine. The corresponding quinazolinone derivatives (5a-e) were obtained by reacting 3a-e with isonicotinic acid hydrazide (4). Both sets of compounds were evaluated for their anti-inflammatory, analgesic effects, and ulcerogenicity in animal models. Structural characterization was performed using spectral analysis. Among the benzoxazinone derivatives, compound 2-(2-((2,6-dichlorophenyl) amino) benzyl)-4H-benzo[d][1,3]oxazin-4-one (3d) exhibited significant anti-inflammatory activity (62.61% inhibition of rat paw edema) and analgesic activity (62.36% protection in acetic acid-induced writhings) with tolerable gastrointestinal toxicity (2.67 ulcerogenicity index) compared to quinazolinone derivatives. The results of antiinflammatory and analgesic activities of both the series are comparable with the respective, positive control. Compound 3d, a benzoxazinone-diclofenac hybrid, emerged as a lead molecule with potent anti-inflammatory, analgesic activities and moderate gastric toxicity showcasing the promising potential for further development. [ABSTRACT FROM AUTHOR]

Published
2024
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8. Silver nanoparticles from Saudi and syrian black cumin seed extracts: Green synthesis, ADME, toxicity, comparative research, and biological appraisal.

Author

Rashid, Mohammad, Athar, Md, Abdelmageed, Mohammed, M Al-Harbi, Mohammed, Husain, Asif, Bisht, Dheeraj, and Kant Arya, Rajeshwar

Subjects
BLACK cumin, SILVER nanoparticles, ESCHERICHIA coli, ANALYSIS of colors, SUSTAINABLE chemistry
Abstract

Objective: The current study's objective is to highlight the value of using plant resources to identify key bioactive molecules and implement green chemistry in research and development to meet market demand. Materials and Methods: The black cumin seeds (Saudi and Syria originated) were utilized to make silver nanoparticles (Ag-NPs), which were subsequently confirmed using a UV spectrophotometer and color analysis of reaction mixtures. The antibacterial activity of Ag-NPs was tested against E. coli, K. pneumoniae, and S. aureus, and antioxidant activity was measured using the DPPH assay. Swiss-ADME, pkCSM, and ProTox-II were also used to assess the pharmacokinetics, oral bioavailability, toxicity, and safety endpoints of molecules. Result: The antibacterial effect of Ag-NPs from Saudi-origin black cumin seeds was observed higher. In comparison to the standard, the Saudi and Syrian Ag-NPs combined displayed synergistic antibacterial effects and were found to be more susceptible to S. aureus. In comparison to the reference, the antioxidant activity of Ag-NPs indicated 60–85% radical scavenging. All molecules passed the Lipinski rule, the filter (Veber, Egan, and Muegge), PAINS, and the Brenk structural alert (zero violations), and the synthetic score was also found to be in the easy limit (1 to 2). The compounds were found to be non-substrate for p-glycoprotein, high GIA% (>90%), non-inhibitor for CYP3A4, CYP2C19, CYP2C9, CYP2D6 (except 5 and 10), Log Po/w (1.71 to 3.26), TPSA 150 2 and MR 155. The compounds likewise had high Caco2 values (log Papp >0.9) with the exception of 4 and 9 (log Papp 0.9), were non-inhibitors of P-gp-I and II and hERG I and II, and showed no AMES toxicity. Except for molecule 11, no organ damage (hepatotoxicity) or endpoint toxicity (mutagenicity, immunotoxicity, carcinogenicity, and cytotoxicity) was identified in ProTox-II. Conclusion: The current study sheds new light on the significance of bioactive molecules found in black cumin seeds, with molecules 3 and 6 identified as potential leads (highest GIA%, no AMES toxicity, oral rat acute and chronic toxicity, lack of renal OCT2 substrate, high total clearance, and lack of organ toxicity) for further research for a variety of medical applications. [ABSTRACT FROM AUTHOR]

Published
2023
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9. A review on alternative methods to experimental animals in biological testing: Recent advancement and current strategies.

Author

Husain, Asif, Meenakshi, Dhanalekshmi, Ahmad, Aftab, Shrivastava, Neelima, and Khan, Shah

Subjects
ANIMAL experimentation, LABORATORY animals, RESEARCH methodology, MOLECULAR biology, RESEARCH personnel
Abstract

With an increase in the progression of research and development in the medical field, the experimental use of animals for the efficacy and safety testing of pharmaceuticals is on rise. Every year, millions of animals are used for experimental testing during which these suffer from pain and are then eventually sacrificed. Besides bioethical issues, animal experimentation is associated with many disadvantages like high cost, the requirement of skilled manpower, approval, and is time-consuming. Therefore, attempts have been made by researchers to design and develop a number of alternative methods that could bypass animal experiments. These methods not only give accurate results but can also save lives of millions of animals annually. Research techniques, including computer and robotics together with molecular biology techniques, are applied to discover new methods to replace animal testing. Several alternative methods are discussed in this review. Some of these methods can predict the behavior of drugs accurately and are as reliable as in-vivo animal models. Furthermore, these alternative methods offer a variety of advantages over experimental animals. However, there is still a great need to discover and develop new, accurate, and reliable methods to replace experimental animals. [ABSTRACT FROM AUTHOR]

Published
2023
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10. Effects of Chemicals Exposure on the Durability of Geopolymer Concrete Incorporated with Silica Fumes and Nano-Sized Silica at Varying Curing Temperatures.

Author

Paruthi, Sagar, Rahman, Ibadur, Husain, Asif, Hasan, Mohd Abul, and Khan, Afzal Husain

Subjects
CONCRETE durability, SILICA fume, CONCRETE additives, FLY ash, CHEMICAL resistance, TEMPERATURE, EFFECT of temperature on concrete
Abstract

Durable concrete significantly reduces the spalling caused by chemical damage. The objective of current research is to substitute cement with supplementary such as fly ash (FA), ground granulated blast furnace slag (GGBS), and alccofine (AF). Additionally, the impact of nano-silica (NS) and silica fumes (SF) on the GPC durability when cured at various temperatures has been attempted. In order to perform this, GPC samples were produced by combining NS and SF at proportions of 0.5% NS + 5% SF, 1% NS + 10% SF, and 1.5% NS + 15% SF, and then cured at temperatures of 27 °C, 60 °C, 90 °C, and 120 °C, respectively. In this research, all concrete specimens were continuously immersed for twelve weeks under four different chemicals, i.e., HCl (2%), H2SO4 (2%), NaCl (6%), and Na2SO4 (6%). The influence of chemical attack on the qualities of concrete was examined by evaluating the water absorption, sorptivity, loss of mass, and loss of GPC strength. The durability aspect is also studied by visual appearance and mass loss under harmful chemical attack. The combination of GPC with integrated NS and SF affords great resistance against chemical attacks. The percentages of these two components are 1.5% and 15%. For GPC specimens, when cured at 90 °C, the resultant strength is found at its maximum. [ABSTRACT FROM AUTHOR]

Published
2023
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11. Development of a Novel Red Clay-Based Drug Delivery Carrier to Improve the Therapeutic Efficacy of Acyclovir in the Treatment of Skin Cancer.

Author

Francis, Arul Prakash, Ahmad, Aftab, Nagarajan, Sri Durga Devi, Yogeeswarakannan, Harish Sundar, Sekar, Krishnaraj, Khan, Shah Alam, Meenakshi, Dhanalekshmi Unnikrishnan, Husain, Asif, Bazuhair, Mohammed A., and Selvasudha, Nandakumar

Subjects
DRUG carriers, SKIN cancer, TREATMENT effectiveness, CANCER cell growth, CANCER treatment
Abstract

Acyclovir (ACV) is a promising candidate for drug repurposing because of its potential to provide an effective treatment for viral infections and non-viral diseases, such as cancer, for which limited treatment options exist. However, its poor physicochemical properties limit its application. This study aimed to formulate and evaluate an ACV-loaded red clay nanodrug delivery system exhibiting an effective cytotoxicity. The study focused on the preparation of a complex between ACV and red clay (RC) using sucrose stearate (SS) (nanocomplex F1) as an immediate-release drug-delivery system for melanoma treatment. The synthesized nanocomplex, which had nanosized dimensions, a negative zeta potential and the drug release of approximately 85% after 3 h, was found to be promising. Characterization techniques, including FT-IR, XRD and DSC-TGA, confirmed the effective encapsulation of ACV within the nanocomplex and its stability due to intercalation. Cytotoxicity experiments conducted on melanoma cancer cell lines SK-MEL-3 revealed that the ACV release from the nanocomplex formulation F1 effectively inhibited the growth of melanoma cancer cells, with an IC50 of 25 ± 0.09 µg/mL. Additionally, ACV demonstrated a significant cytotoxicity at approximately 20 µg/mL in the melanoma cancer cell line, indicating its potential repurposing for skin cancer treatment. Based on these findings, it can be suggested that the RC-SS complex could be an effective drug delivery carrier for localized cancer therapy. Furthermore, the results of an in silico study suggested the addition of chitosan to the formulation for a more effective drug delivery. Energy and interaction analyses using various modules in a material studio demonstrated the high stability of the composite comprising red clay, sucrose stearate, chitosan and ACV. Thus, it could be concluded that the utilization of the red clay-based drug delivery system is a promising strategy to improve the effectiveness of targeted cancer therapy. [ABSTRACT FROM AUTHOR]

Published
2023
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12. Anticancer heterocyclic hybrids: design, synthesis, molecular docking and evaluation of new thiazolidinone-pyrazoles.

Author

Shrivastava, Neelima, Khan, Shah Alam, Alam, Mohammad Mumtaz, Akhtar, Mymoona, Srivastava, Apeksha, and Husain, Asif

Subjects
MOLECULAR docking, ANTINEOPLASTIC agents, CHEMICAL synthesis, CELL lines, PYRAZOLES
Abstract

In order to obtain potential anticancer agents, hybrid compounds have been synthesized by coupling thiazolidinone and pyrazole scaffolds. Among the synthesized compounds, 2-(1,3-diphenyl-1H-pyrazol-4-yl)-3-phenyl thiazolidin-4-one (4a) was found to be the most potent based on a docking (−9.307) and binding scores (−66.46), along with good ADME parameters. In vitro anticancer activity of compound 4a shows a maximum inhibition against lung cancer (NCI-H23) cell lines with a moderate inhibition rate of 31.01%. Molecular docking studies revealed that these hybrid compounds bind well to the active site of peroxisome proliferator-activated receptors-gamma (PPAR-gamma). Doxorubicin was used as a positive control. It can be concluded that 4a having pyrazole-thiazolidinone ring systems has the potential to be developed as an anticancer agent. [ABSTRACT FROM AUTHOR]

Published
2023
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13. Synthesis, and reverse screening of 6‐(3,4,5‐trimethoxyphenyl)pyrimidine‐5‐carbonitrile derivatives as anticancer agents: Part‐II.

Author

Nainwal, Lalit Mohan, Shaququzzaman, Mohammad, Akhter, Mymoona, Husain, Asif, Parvez, Suhel, Tasneem, Sharba, Iqubal, Ashif, and Alam, Mohammad Mumtaz

Subjects
ANTINEOPLASTIC agents, CELL lines, COLON cancer, CANCER cells, PYRIMIDINES
Abstract

In continuation to our previous studies on cyanopyrimidine derivatives as anticancer agents, we further designed, synthesized, and evaluated new 3,4,5‐trimethoxy phenyl ring pendant sulfur‐containing cyanopyrimidine derivatives (4a–m) with a particular lipophilic behavior. In this work, we have varied the chain length from isopropyl to isopentyl and evaluated their anticancer activities. To study the antiproliferative spectrum, in vitro evaluation was piloted against a panel of 60 cancer cell lines at the National Cancer Institute, United States. Compound 4g (NSC: D‐813664) displayed the most promising broad‐spectrum anticancer activity with high growth inhibition of various cell lines representing action against multiple cancers diseases. It showed percentage growth inhibition of 84.01 and 76.94 against SR leukemia and HCT‐116 colon cancer cell lines. Absorption, distribution, metabolism, excretion, and toxicity studies and reverse screening were also performed to identify the potential targets of designed molecules. It was concluded that 6‐(3,4,5‐trimethoxyphenyl) pyrimidine‐5‐carbonitrile derivatives exhibited its anticancer activity through different targets and hence could be further structurally modified and optimized to develop more potent multi‐targeting anticancer agents. [ABSTRACT FROM AUTHOR]

Published
2022
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14. Furanone-functionalized benzothiazole derivatives: synthesis, in vitro cytotoxicity, ADME, and molecular docking studies.

Author

Husain, Asif, Bedi, Silky, Parveen, Shazia, Khan, Shah Alam, Ahmad, Aftab, Iqbal, Md Azhar, Farooq, Aasif, and Ahmed, Anwar

Subjects
BENZOTHIAZOLE derivatives, CYTOTOXINS, MOLECULAR docking, ANTINEOPLASTIC agents, CELL lines, LEAD compounds, DRUG standards, BENZOXAZOLES
Abstract

In the present study, a novel series of new furanone-based benzothiazole derivatives (4a-j) were synthesized from 4-(benzo[d]thiazol-2-yl)-4-oxobutanoic acid (3) as potential anticancer agents. In vitro cytotoxicity against three human cancer cell lines (A549, MCF7, and DUI45) revealed substantial activity. Di-substituted compound, 4i emerged as a promising anticancer compound which showed IC50 values of 7.2 ± 0.5, 6.6 ± 1.4, and 7.3 ± 0.1 µM against A549, MCF7, and DUI45 cell lines, respectively. Four compounds 4c, 4e, 4f, and 4i evaluated for their acute toxicity were found to be non-toxic on the two vital organs (liver and heart). Further, these compounds were found to be more efficient and less hepatotoxic in comparison to standard drug doxorubicin. Molecular docking studies carried out with VEGFR-2 revealed compounds 4a and 4i as potential VEGFR-2 kinase inhibitors. In silico ADME evaluation was carried out to estimate and predict drug-likeness. Compound 4i demonstrated the best ADME parameters. Based on the results of docking analyses, ADME, and in vitro cytotoxicity, compound 4i is identified as the lead compound for further development of anticancer agents. [ABSTRACT FROM AUTHOR]

Published
2022
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15. APPROACHES FOR CHEMICAL SYNTHESIS AND DIVERSE PHARMACOLOGICAL SIGNIFICANCE OF PYRAZOLONE DERIVATIVES: A REVIEW.

Author

ASIF, MOHAMMAD, IMRAN, MOHD, and HUSAIN, ASIF

Subjects
CHEMICAL synthesis, PYRAZOLONES, LACTAMS, CEREBRAL ischemia, ANTI-infective agents, ANTIPYRINE
Abstract

Pyrazolone is a five-membered lactam ring containing two Nitrogens and one ketonic group in its structure. Numerous pyrazolone derivatives were exhibited with diverse biological, pharmacological, and chemical applications. When pyrazolones were discovered, they were only known as NSAIDs but in recent times they play a versatile role in several complications like cerebral ischemia, cardiovascular diseases, antibacterial, antioxidant, anticancer and several other pharmacological activities. Over the last few decades, pyrazolone derivatives have been used for various biochemical applications. Some of these derivatives such as metamizole, phenazone, aminopyrine, and propyphenazone, are widely used as anti-inflammatory and analgesics. The chemistry of pyrazolone has gained increasing attention due to its diverse pharmacological properties such as anticancer, analgesic, anti-inflammatory, antimicrobial, antioxidant, antifungal, antiviral, antidiabetic, and several other biological activities. Thus, keeping because of their importance, synthetic strategies for existing as well as novel pyrazolone derivatives have been developed and explored their biochemical utility. This review deals with the various pharmacological properties of different pyrazolone derivatives and puts chemical synthetic schemes. [ABSTRACT FROM AUTHOR]

Published
2021
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16. A review on synthetic procedures and applications of phosphorus oxychloride (POCl3) in the last biennial period (2018–19).

Author

Amin, Shaista, Alam, M. Mumtaz, Akhter, Mymoona, Najmi, A. K., Siddiqui, Nadeem, Husain, Asif, and Shaquiquzzaman, M.

Subjects
PHOSPHORUS, ORGANIC synthesis, CHLORINATION, RING formation (Chemistry), DEHYDRATION reactions, DEHYDRATION
Abstract

Phosphorus oxychloride, POCl3, an important phosphorus compound, has diverse applications in synthetic chemistry. It plays an important role in chlorination, Vilsmeier Haack reaction, dehydration and cyclization which have been highlighted here. Moreover, different reaction conditions implied and reported in the literature along with the general mechanism are provided briefly in this review. This review provides an insight into the recent applications of phosphorus oxychloride as a reagent in organic syntheses in the last two year i.e. 2018–19. [ABSTRACT FROM AUTHOR]

Published
2021
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17. Synthesis, in vitro cytotoxicity, ADME, and molecular docking studies of benzimidazole‐bearing furanone derivatives.

Author

Husain, Asif, Bhutani, Medha, Parveen, Shazia, Khan, Shah Alam, Ahmad, Aftab, and Iqbal, Md Azhar

Subjects
MOLECULAR docking, BENZIMIDAZOLES, VASCULAR endothelial growth factor receptors, FURANONES
Abstract

A series of benzimidazole‐derived–furanones (4a–l) were synthesized, characterized, and explored for their in vitro anticancer activities. The pharmacokinetic parameters assessed revealed that all the compounds followed the Lipinski's rule of five, making them potential drug candidates. Further, the results of anticancer activity revealed that (E)‐5‐(1H‐benzo[d]imidazol‐2‐yl)‐3‐(3,4,5‐trimethoxybenzylidene)furan‐2(3H)‐one (4a), was active against A549, MCF7, and DU145 with an IC50 values of 10.4 ± 0.39, 11.1 ± 0.43, and 10.7 ± 0.19 μM, respectively. While another compound (E)‐5‐(1H‐benzo[d]imidazol‐2‐yl)‐3‐([5‐phenyl]furan‐2‐yl)furan‐2(3H)‐one (4k) also exhibited good activity against A549, MCF7, and DU145 with IC50 values of 11.4 ± 0.39, 9.1 ± 0.43, and 12.7 ± 0.19 μM, respectively. Doxorubicin was used as the standard drug. Further, molecular docking studies were carried out to provide binding mode into the binding sites of vascular endothelial growth factor receptor (VEGFR). Docking scores and binding energies corroborated well with the results of experimental anticancer activity. Pharmacokinetic (ADME) parameters of the potent derivatives were also found to be in an acceptable range. The benzimidazole‐furanonone conjugates seem to be a potential source for the further development of potent cytotoxic agents. [ABSTRACT FROM AUTHOR]

Published
2021
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20. SYNTHESIS AND SAR STRATEGY OF THIAZOLIDINEDIONE: A NOVEL APPROACH FOR CANCER TREATMENT.

Author

RASHID, MOHAMMAD, SHRIVASTAVA, NEELIMA, and HUSAIN, ASIF

Subjects
THIAZOLIDINEDIONES, ANTINEOPLASTIC agents, STRUCTURE-activity relationship in pharmacology, HETEROCYCLIC compounds synthesis, PROTEIN-tyrosine kinase inhibitors
Abstract

In current review, authors aim to inspire the researcher through structure activity relationship strategy for the finding of safe and effective anticancer molecules. Nowadays cancer is measured as one of the major health problems in human beings in the world from decades. A classes of heterocyclic compounds have been recognized through molecular biology, empirical screening and rational drug development for the evaluation of anticancer mole cules however regrettably, till now we could not find a medicine to be entirely active and nontoxic for the treatment of cancer patients. In pointed view, it might be measured that Thiazolidinedione (TZD) heterocyclic compounds are prodigious standing in the synthetic and pharmacological approach of medicinal chemistry. Thiazolidinedione (TZD) nucleus upon the substitution of various functional groups is provides a wide spectrum of biological activity by the use of different mechanism on d ifferent target sites. Recently, some of the substituted thiazolidinedione molecules are designed for the treatment of human cancers cell line through different molecular mechanism such as EGFR & Mushroom Tyrosine kinase inhibitor, COX enzyme inhibitors, Histone deacetylase inhibitors, Alpha glucosidase inhibitor, DNA intercalation and Protein tyrosine phosphatase 1B (PTP1B) inhibitor, basically in which PPAR gamma express are in high levels. Peroxisome proliferator-activated receptor (PPAR) gamma ligands effect on apoptosis, cell proliferation and cell differentiation on different types of cell. The most commonly cascades in human cancers cell are Raf/MEK/ERK, Wnt and PI3/Akt. This article highlights and embraces a concise overview of recent approaches for the synthesis of new thiazolidinedione molecules with its structure activity relationship strategy and effects on various signaling pathways, which is responsible for the expresses of cancer cell line activity. [ABSTRACT FROM AUTHOR]

Published
2020
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21. Standardization of Diminutive Specimen Testing Techniques for Predicting the Mechanical Properties of Metals.

Author

Hafeez, Farrukh and Husain, Asif

Subjects
MECHANICAL properties of metals, STANDARDIZATION, MATERIALS testing, CUTTING machines, TEST methods
Abstract

The present paper intends to standardize the miniature test results obtained from the testing of a ring shaped miniature specimen having a V notch placed at diametrically opposite ends of the ring. The rings of 0.5mm, 0.8mm and 1.0mm thickness were sliced from these circular rods on EDM wire cut machines. A V-shaped notch of 1mm depth and 60° angle of cut was developed manually on all rings, along same diametrically opposite ends, using a fine grade triangular cross cut file. A Vnotch is being added diametrically to obtain both the uniaxial mechanical properties and fracture properties from the same test. The procedure for making this specimen is easier as compared to that of making conventional sub size tension test specimens. The test techniques and various formulations performed on different shape, sizes and material specimen has been adopted as a standards. The results can best be implemented as an alternative for the conventional test methods, for predicting the mechanical properties of in-service components or structures where the availability of material is limited and conventional test methods cannot be used without loss of significant amount of material. Diminutive uniaxial tests are not yet standardized with the exception of some requirements for testing foil materials as provided in ASTM E345-93 but the micro testing method have the potential to provide uniaxial stress strain data that can be correlated to macro behavior. Testing parameters, such as specimen geometry, specimen preparation methods, micro structural changes, alignment, ductility, resolution of load cells and strain measuring devices greatly influences the test results. The exhaustive research in the miniature specimen analysis is intended to formulate conversion relationships and standardize the miniature test results irrespective of the specimen equivalent gauge length (EGL) or L/W ratio, sensitivity to specimen geometry, specimen size, thickness and material. [ABSTRACT FROM AUTHOR]

Published
2019
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22. IDENTIFICATION, ISOLATION AND CHARACTERIZATION OF ALKALINE DEGRADATION PRODUCT OF ESLICARBAZEPINE ACETATE.

Author

Iram, Farah, Siddiqui, A. A., Ahmad, Aftab, Khan, S. A., and Husain, Asif

Subjects
ACETATES, ANTICONVULSANTS
Abstract

Eslicarbazepine acetate (ESA) a potent sodium channel blocker and an antiepileptic drug were subjected to various stress conditions as recommended by ICH guideline which includes hydrolytic, oxidative, thermal, and photolytic stress. The degradation studies show that ESA degraded in alkaline hydrolytic condition only while it found to be stable in other stressed conditions. A single degradation product emerged in UPLC studies on Waters Acquity BEH 150 x 2.1 mm, 1.7 µm, C18 column using mobile phase A (0.01M potassium dihydrogen orthophosphate and acetonitrile; 90:10 v/v) and mobile phase B (acetonitrile-watermethanol; 75:5:25 v/v) in the ratio of 50:50 (v/v) at RT 1.83 min with 0.2 ml/min flow rate and 2µl injection volume. The obtain degradation product from Eslicarbazepine acetate was isolated and characterized by IR, 1HNMR and UPLC-MS/MS analytical techniques. IR evaluation exhibited peaks at 3475.73 cm-1, 3363.86 cm-1, 1726.29 cm-1 for O-H, COO-H and C=O group, respectively. 1H NMR spectrum showed singlet at 11.865 which indicated the presence of COOH group. UPLC-MS/MS analysis shows molecular ion peak at 255.2 m/z. The recognized peak in the obtained spectrum confirmed the structure of the degradation product as 10-hydroxy-10,11-dihydro-5H-dibenzo[b,f]azepine-5-carboxylic acid which was formed by alkaline hydrolytic degradation. [ABSTRACT FROM AUTHOR]

Published
2019
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23. Syntheses and Pharmacological Activities of Isatin Derivatives.

Author

Yadav, Mayank, Sachan, Neetu, Kumar, Sushil, and Husain, Asif

Subjects
ISATIN, GRAM-positive bacteria, GRAM-negative bacteria, PENICILLIUM chrysogenum, RHIZOPUS oryzae
Abstract

Twenty derivatives of isatin (1H-indole-2, 3-Dione) were synthesized by the schematic route as per as scheme. These were further characterized by spectroscopic analysis. All the novel synthesized derivatives of isatin were screened for their antimicrobial activity against Gram-positive bacteria: Staphylococcus aureus, Bacillus subtilis, Streptococcus pneumonia; Gram-negative bacteria: Escherichia coli, Pseudomonas aeruginosa, Klebsiella pneumoniae and fungal strains: Candida albicans, Aspergillus niger, Penicillium chrysogenum, Rhizopus oryzae by cup-plate method. Results of antimicrobial screening showed that compound ID5, ID9, ID15 and ID18 possess potent antibacterial activity. Whereas ID1, ID3, ID4, ID7 and ID20 possess antifungal activity comparable to standard drugs. [ABSTRACT FROM AUTHOR]

Published
2019
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24. Studies on Chromene based 2, 6-disubstituted-Thiazolo [3,2-B] [1,2,4] Triazole derivatives: Synthesis and Biological Evaluation.

Author

Naseer, Md Arif and Husain, Asif

Subjects
TRIAZOLE derivatives, BIOSYNTHESIS, DRUG standards, PHOSPHORIC acid, ISOXAZOLES, IBUPROFEN
Abstract

In this study, a series of novel chromene based 2,6-disubstituted-thiazolo[3,2-b] [1,2,4] triazole derivatives (7a-g) were synthesized by condensing 5-substituted-1,2,4-traizole-thione (6a-g) using poly phosphoric acid through one pot reaction. The structure of new compounds was supported by 1H NMR, 13C NMR and MS data. The synthesized compounds were evaluated using writhing assays for analgesic and carrageenan-induced rat paw edema method for anti-inflammatory activities respectively. Some of the newly synthesized compounds 7c, 7f and 7g showed very good anti-inflammatory activity with 90.83%, 85.81% and 88.40% protection respectively along with low GI toxicity as compared to standard drug ibuprofen while compounds 7a, 7b, 7d and 7f showed highest analgesic activity with 52.54%, 54.02%, 56.76% and 52.45% protection among them compound 7d showed better protection than standard drug ibuprofen. [ABSTRACT FROM AUTHOR]

Published
2019
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25. Synthesis, Computational Studies and Anticonvulsant Activity of Novel Benzothiazole Coupled Sulfonamide Derivatives.

Author

Khokra, Sukhbir L., Arora, Kanika, Khan, Shah A., Kaushik, Pawan, Saini, Reetu, and Husain, Asif

Subjects
ANTICONVULSANTS, BENZOTHIAZOLE derivatives, SULFONAMIDES, NEUROTOXICOLOGY, PHENYL group
Abstract

We report herein the synthesis of ¾ substituted benzene sulfonamides linked via phenyl ring to a benzothiazole moiety. The title compounds in the two series namely N-(4-(benzothiazole-2-yl) phenyl) 4-substituted benzene sulfonamides and N-(4-(benzothiazole-2-yl) phenyl) 3-substituted benzene sulfonamides were synthesized by condensing 2-(3/4-aminophenyl) benzothiazole with various substituted sulfonyl chlorides. The synthesized compounds were subjected to neurotoxicity screening, computational studies, and evaluation of their anticonvulsant potential. Amongst all the synthesized compounds, compound 9 emerged as the most potent anticonvulsant agent in maximal electroshock (MES) model (standard: phenytoin) in mice and showed three hydrogen bond interactions with the nicotinic acetylcholine ion gated receptors (PDB ID: 2BG9). Interestingly, compound 13 showed five hydrogen bond interactions with the target protein and thus excellent binding affinity upon computational analysis but was found to be neurotoxic. [ABSTRACT FROM AUTHOR]

Published
2019

26. Newly Synthesized Oxadiazole Based Mannich Base Derivatives of Fatty Acid: In silico Study and In vivo Anti-Hyperglycaemic Estimation.

Author

KAPOOR, GARIMA, PATHAK, DHARAM PAL, BHUTANI, RUBINA, HUSAIN, ASIF, JAIN, SANDEEP, KANT, RAVI, and IQBAL, MD. AZHAR

Subjects
OXADIAZOLES, FATTY acid derivatives, PEROXISOME proliferator-activated receptors, MOLECULAR docking, BINDING energy, STREPTOZOTOCIN
Abstract

A receptor peroxisome proliferator activated receptor-gamma was targeted by series of new fatty acid chemical entities (M1-M22) which was designed, synthesized and characterized by spectral analysis. Metabolites molecular properties were calculated using Lipinski's rule of five using molinspiration online software. Docking studies were done on co-crystallized protein structure of PPAR γ, PDB-1FM9 showing M15, M17 and M8 to be best located in the active sites with scores -10.43, -10.21 and -10.00 respectively. The free binding energy estimation was done using model of Maestro 9.0 (Schrodinger) and lies between -80.15 to -61.26 kcal/mol which is significant as compared to that of standard (-48.58 Kcal/mol). Nine best docked derivatives were evaluated in-vivo for oral glucose tolerance and antihyperglycemic activity by streptozotocin induced diabetes model and M15 exhibited most promising antidiabetic activity more than the standard glibenclamide. The promising results encourage future investigation on fatty acids for development of active compounds. [ABSTRACT FROM AUTHOR]

Published
2018
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27. Ameliorative Effect of Camel's Milk and Nigella Sativa Oil against Thioacetamide-induced Hepatorenal Damage in Rats.

Author

Ahmad, Aftab, Al-Abbasi, Fahad, Sadath, Saida, Ali, Soad, Abuzinadah, Mohammed, Alhadrami, Hani, Mohammad Alghamdi, Anwar, Aseeri, Ali, Khan, Shah, and Husain, Asif

Subjects
HEPATORENAL syndrome, BLACK cumin, CAMEL milk, KIDNEY function tests, LIVER function tests, HISTOPATHOLOGY, THERAPEUTICS
Abstract

Background: Camel milk (CM) and Nigella sativa (NS) have been traditionally claimed to cure wide range of diseases and used as medicine in different part of world, particularly in Saudi Arabia. Several research studies have been published that proved beneficial effects of CM and NS. Objective: This study was undertaken to investigate the antihepatotxic potential of CM and NS oil (NSO) against thioacetamide (TAA)-induced hepato and nephrotoxicity in rats. Materials and Methods: Thirty female Albino Wistar rats were randomly divided in to six groups having five rats in each group. A single subcutaneous injection of TAA (100 mg/kg b. w.) was administered to all the rats in Group-II to VI on 1st day to induce hepatorenal damage. Group I served as a normal control while Group II served as toxic control for comparison purpose. Experimental animals in Group III, IV, and V were supplemented with fresh CM, (250 mL/24 h/cage), NSO (2 mL/kg/day p. o.), and NSO + fresh CM, respectively. Group VI was treated with a polyherbal hepatoprotective Unani medicine Jigreen (2 mL/kg/day p. o.) for 21 days. TAA-induced hepatorenal damage and protective effects of CM and NSO were assessed by analyzing liver and kidney function tests in the serum. Histopathology of liver and kidney tissues was also carried out to corroborate the findings of biochemical investigation. Results: The results indicated that the TAA intoxicated rats showed significant increase in the alanine transaminase, aspartate transaminase, gamma-glutamyl transpeptidase, alkaline phosphatase, lipid profile, urea, creatinine, uric acid, sodium, and potassium levels in serum. Treatment of rats with CM, NSO, and CM plus NSO combination and Jigreen significantly reversed the damage and brought down the serum biochemical parameters and lipid profile toward the normal levels. The histopathological studies also support the hepato and nephroprotective effects of CM and NSO. Conclusion: This study demonstrated the ameliorative effects of CM, NSO, and CM plus NSO combination against TAA-induced hepatorenal toxicity in rats. [ABSTRACT FROM AUTHOR]

Published
2018
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28. Eslicarbazepine acetate: A therapeutic agent of paramount importance in acute anticonvulsant therapy.

Author

Iram, Farah, Khan, Shah Alam, Ahmad, Aftab, Siddiqui, Anees A., and Husain, Asif

Subjects
TREATMENT of epilepsy, ANTICONVULSANTS, DRUG efficacy, VOLTAGE-gated ion channels, CLINICAL drug trials
Abstract

Eslicarbazepine acetate (ESL) is a new, once daily, orally administered, third generation antiepileptic drug which is indicated in the treatment of partial-onset seizures. ESL is known to exert it's anticonvulsant effect by blocking the voltage-gated sodium channels. Several clinical trials and pharmacological studies have revealed that seizure control was better with ESL monotherapy (1 200 or 1 600 mg once daily) following a switch from other antiepileptic drugs in comparison with pseudo-placebo patients. The studies have indicated the ESL to be well tolerated and produced only mild to moderate emergent adverse events with the therapy. Being a dibenzazepine family member, structure and chemistry of ESL resembles more or less to carbamazepine and oxcarbazepine. ESL differs structurally from carbamazepine and oxcarbazepine at the 10, 11 position of dibenazepine nucleus. This molecular variation results in differences in metabolism and thus helps to prevent the formation of toxic epoxide metabolites. ESL following oral administration is rapidly metabolised to active metabolite namely S-licarbazepine which is responsible for its pharmacological activity. ESL exhibits acceptable pharmacokinetic profile and shows insignificant drug-drug interactions. In phase III clinical program, ESL was found to be efficacious and well tolerated in adult patients with partial onset seizures previously not controlled with treatment with one or two other antiepileptic drugs. [ABSTRACT FROM AUTHOR]

Published
2017
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29. Oxidative Cyclization of Isoniazid with Fluoroquinolones: Synthesis, Antibacterial and Antitubercular Activity of New 2,5-disubstituted-1,3,4-Oxadiazoles.

Author

Khan, Shah Alam, Ahuja, Priyanka, and Husain, Asif

Subjects
ISONIAZID, RING formation (Chemistry), FLUOROQUINOLONES, CHEMICAL synthesis, ANTIBACTERIAL agents, ANTITUBERCULAR agents, OXADIAZOLES
Abstract

We report herein one-pot synthesis and the antibacterial and antitubercular activities of 2,5-disubstituted-1,3,4-oxadiazole compounds obtained by hybridization of a well-known antitubercular agent isoniazid ( INH) with four broad-spectrum antibiotics belonging to fluoroquinolone ( FQ) class. The work is aimed at designing and developing potential antimicrobial agents having synergistic action due to the coupling of INH and FQ through the biologically active 1,3,4-oxadiazole nucleus. The synthesized compounds are expected to have low toxicity as compared to INH due to the absence of free hydrazide group in the chemical structure of the prepared derivatives. The antibacterial activities of the 1,3,4 oxadiazole derivatives were also tested against several Gram-positive and Gram-negative pathogenic bacterial strains. The antitubercular activity was evaluated against M. tuberculosis H37Rv strain, and the results were compared with that of the positive control INH. The title compounds showed excellent antimicrobial and promising antitubercular activity in comparison to the parent fluoroquinolones and INH, respectively. [ABSTRACT FROM AUTHOR]

Published
2017
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31. Synthesis and in vivo diuretic activity of some new benzothiazole sulfonamides containing quinoxaline ring system.

Author

Husain, Asif, Madhesia, Diwakar, Rashid, Mohd, Ahmad, Aftab, and Khan, Shah Alam

Subjects
CHEMICAL synthesis, BENZOTHIAZOLE, SULFONAMIDES, QUINOXALINE compounds, CYCLIC compounds, SUBSTITUENTS (Chemistry), IN vivo studies
Abstract

A series of new 6-substituted-N-[3-{2-(substituted phenyl)-ethenyl} quinoxaline-2(1H)-ylidene]-1,3-benzothiazole-2-amine (4a–f) were designed and synthesized by condensing 2-amino-benzothiazole-6-sulfonic acid amide (1) with chalcones of quinoxaline-2-one (3a–f) in a hope to obtain promising and a new class of diuretic agents. Structures of all the newly synthesized compounds were characterized by spectral data and elemental analysis. The pharmacological studies in experimental rats indicates that compound4cpossesses excellentin vivodiuretic activity of 1.13 and appears to be a better diuretic agent than the reference drugs, acetazolamide (1.0) and urea (0.88). Insight of the binding mode of the synthesized compounds (ligand) into the binding sites of carbonic anhydrase enzyme (PDF code: 4KUV) was provided by docking studies, performed with the help of Maestro 9.0 docking software. Further pharmacokinetic and toxicological studies are needed to confirm the safety of compound4cwhich emerged as a lead diuretic compound. [ABSTRACT FROM PUBLISHER]

Published
2016
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32. Synthesis, Molecular Docking and Potential Antioxidant Activity of Di/Trisubstituted Pyridazinone Derivatives.

Author

Khokra, Sukhbir Lal, Khan, Shah Alam, Thakur, Pramila, Chowdhary, Deepika, Ahmad, Aftab, and Husain, Asif

Subjects
PYRIDAZINONES, BENZYLIDENE compounds, ANTIOXIDANT analysis, ANALYSIS of hydrogen peroxide, VITAMIN C deficiency, OXIDOREDUCTASE genetics
Abstract

A number of pyridazinone derivatives bearing substituted benzylidene and heterocyclic/aromatic rings at 4th and 6th positions, respectively were synthesized in good to moderate yields and screened for antioxidant activity. Antioxidant activity of pyridazinone derivatives was evaluated by using several in vitro radical scavenging methods such as 1,1-diphenylpicrylhydrazyl (DPPH), hydrogen peroxide (H2O2), nitric oxide (NO), reducing power, and metal chelating assay etc. Molegro virtual docker software was used to study the binding affinity of the title compounds with the xanthine oxidoreductase enzyme. Amongst the tested compounds, 5a, 5d, 5g & 5j were found to exhibit excellent antioxidant activity at par with the positive control, ascorbic acid. The molecular docking studies of these compounds demonstrated a good selectivity profile with xanthine oxidoreductase receptors. A preliminary study of the structural-activity relationship showed that the presence of electron withdrawing group and heterocyclic ring on pyridazinone nucleus are associated with the best potency and selectivity profile. It could be proposed that xanthine oxidoreductase receptor may be involved in observed antioxidant activity of pyridazinone derivatives bearing aromatic ring and benzylidene substituents and thus the synthesized compounds are worthy of further exploration. [ABSTRACT FROM AUTHOR]

Published
2016
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33. A review on dronedarone: Pharmacological, pharmacodynamic and pharmacokinetic profile.

Author

Iram, Farah, Ali, Sadaf, Husain, Asif, Ahmad, Aftab, and Khan, Shah Alam

Subjects
DRONEDARONE hydrochloride, PHARMACOLOGY, PHARMACOKINETICS
Abstract

Dronedarone, a benzofuran containing chemical compound, is a derivative of amiodarone which is classified as a Class III antiarrhythmic agent. It is prescribed to the cardiovascular patients who have paroxysmal or persistent atrial fibrillation to lower the chances of hospitalization. Amiodarone, sotalol, procainamide dofetilide, quinidine, ibutilide, flecainide, and propafenone are the other useful medicinal products used to treat atrial fibrillation or cardiac arrhythmia. Dronedarone was approved for clinical use in atrial fibrillation by the Food and Drug Administration in 2009. The generic name for dronedarone is Multaq (Sanofi Aventis). This article briefly highlights the important pharmacological, pharmacodynamic and pharmacokinetic properties of dronedarone. [ABSTRACT FROM AUTHOR]

Published
2016
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34. Design and synthesis of butenolide-based amide derivatives as anti-inflammatory agents.

Author

Ali, Yakub, Alam, Mohammad, Hamid, Hinna, Husain, Asif, Dhulap, Abhijeet, Bano, Sameena, Kharbanda, Chetna, Nazreen, Syed, and Haider, Saqlain

Abstract

Butenolide-based eighteen new amide derivatives ( 1-18) have been synthesized and evaluated for anti-inflammatory activity. The compounds 9, 17 and 4 exhibited significant in vivo inhibition of 84.69, 76.52 and 76.22 % inflammation, respectively, after 5 h without causing any damage to stomach and liver in comparison with the standard drug indomethacin which showed 79.04 % inhibition. The compounds showing potent anti-inflammatory activity were further evaluated for ex vivo TNF-α suppression. Compounds 9, 17 and 4 significantly suppressed TNF-α concentration to 74.83, 71.74 and 67.11 % as compared to indomethacin which exhibited a suppression of 69.01 %. Compounds 9 and 17 were also found to suppress the expression of COX-2 and NF-κB in the paw tissue. Moreover, compound 9 showed significant analgesic activity (57.03 %) which was comparable to indomethacin (61.03 %). [ABSTRACT FROM AUTHOR]

Published
2015
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35. Design and Synthesis of Butenolide-based Novel Benzyl Pyrrolones: Their TNF- α based Molecular Docking with In vivo and In vitro Anti-inflammatory Activity.

Author

Ali, Yakub, Alam, Mohammad Sarwar, Hamid, Hinna, Husain, Asif, Shafi, Syed, Dhulap, Abhijeet, Hussain, Firasat, Bano, Sameena, Kharbanda, Chetna, Nazreen, Syed, and Haider, Saqlain

Subjects
BUTENOLIDES, TUMOR necrosis factor receptors, MOLECULAR docking, ANTI-inflammatory agents, INDOMETHACIN, LIPID peroxidation (Biology)
Abstract

A focused library of novel benzyl pyrrolones has been synthesized and their in silico molecular docking studies carried out against TNF- α target. Among all the docked molecules, compound 3f showed best glide score of −6.89. All the synthesized compounds were evaluated for in vivo anti-inflammatory activity by carrageenan-induced paw edema model. Compounds showing significant anti-inflammatory activity were further tested for their in vitro TNF α expression. Compounds 3b and 2b were found to show significant inhibition of 76.22% and 71.47%, respectively after 5 h in comparison with standard drug indomethacin, which showed 80.98% inhibition of inflammation. Compounds 3b and 2b also suppressed TNF α level by 65.03% and 60.90% as compared indomethacin, which showed 68.84% of inhibition. Compound 3b showed significant analgesic activity of 60.04%, and its activity was comparable with indomethacin (64.04%). Compounds 3b and 2b were also tested for their effect on protein expression of COX-2 and NF- κB in the liver tissues. Compounds 3b and 2b were further evaluated for their gastric risk and lipid peroxidation action and showed superior GI safety along with reduction of LPO as compared to indomethacin. Hepatotoxicity study showed that these two compounds did not cause any damage to liver. [ABSTRACT FROM AUTHOR]

Published
2015
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36. SYNTHESIS, COMPUTER AIDED SCREENING AND PHARMACOLOGICAL EVALUATION OF 2/3-SUBSTITUTED-6(4- METHYLPHENYL)-4,5-DIHYDROPYRIDAZIN3(2H)-ONES, AND PYRIDAZINE SUBSTITUTED TRIAZINE.

Author

Khokra, Sukhbir Lal, Seth, Sonakshi, Garg, Shama S., Kaushik, Pawan, Ahmad, Aftab, Khan, Shah Alam, and Husain, Asif

Subjects
DRUG use testing, PYRIDAZINES, NONSTEROIDAL anti-inflammatory agents, FRIEDEL-Crafts reaction, SUCCINIC anhydride, PHOSPHORUS oxychloride
Abstract

The present research work involved synthesis of some new pyridazine derivatives and evaluation of their analgesic and antiinflammatory activities in experimental animals to obtain safer non-steroidal anti-inflammatory agents (NSAIDs). Friedel-Crafts acylation reaction of succinic anhydride with toluene in the presence of anhydrous aluminum chloride gave 4-(4- methylphenyl)-4-oxo-butanoic acid (1). The aryl propionic acid 1 on reaction with phenyl hydrazine and hydrazine hydrate yielded the pyridazinone derivative 2 and 3, respectively. Reaction of the compound 3 with phosphorus oxychloride (POCl3) produced the corresponding chloropyridazine derivative 4. A 4-hydroxymethyl derivative of dihydropyridazinone (5) was synthesized by condensing 3 with methanol and formaldehyde (HCHO). The compound 5 on further treatment with guanidine hydrochloride in ethanol gave the pyridazino-triazine (6). The synthesized compounds were investigated for their analgesic activity in mice and anti-inflammatory activity in Wistar albino rats. The molecular, pharmacokinetic and toxicity properties of the synthesized compounds were calculated by Molinspiration and Osiris property explorer software. The results of in-vivo antiinflammatory studies revealed that the compound. 4 showed maximum inhibition in paw edema volume followed by compound 3 while the compound 4 exhibited excellent peripheral analgesic activity (74%) followed by the compound 5. Compound s 4 and 5 also showed good central analgesic effect increased the reaction time to 90 minutes. All the title compounds except compound 5 are predicted to be safe by Osiris online software and are likely to have good oral bioavailability as they obey Lipinski's rule of five for drug likeness. [ABSTRACT FROM AUTHOR]

Published
2015
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38. Essential aminoacid incorporated GABA-phthalimide derivatives: synthesis and anticonvulsant evaluation.

Author

Ahuja, Priya, Husain, Asif, and Siddiqui, Nadeem

Abstract

A series of novel N-(2-(benzylamino)-1-substituted-2-oxoethyl)-4-(1,3-dioxoisoindolin-2-yl)butanamide derivatives were synthesized unifying the functionalized amino acid unit and GABA-phthalimide moiety with essential amino acid substituted on it with a view to explore prospective anticonvulsant candidates. The initial screening was performed using the intraperitoneal (i.p) maximal electroshock test and sub-cutaneous Pentylenetetrazole (scPTZ) test in mice. The neurotoxicity was determined by the minimal motor impairment based on rotarod test. The outcomes established the ability of the compounds to suppress the convulsions generated by electrical seizures. The scPTZ test provided insignificant activity profile. The leads of initial screening ( 4a, 4e and 4g) were subjected to the quantification studies in mice (i.p) and rats (p.o). The quantitative study in mice depicted an increase of 1.7-, 2.3- and 4-fold over phenytoin in the protective index, the keystone in the drug discovery for the anticonvulsant activity. The PI values in rat oral administration were 13.33, >145 and >100 for these compounds, respectively. The gamma-amino butyric acid level in the different brain regions also increased on administration of the active compounds with 4g providing the maximum increment. These results encourage our future investigation on the rational modification of this basic framework for better potency. [ABSTRACT FROM AUTHOR]

Published
2014
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39. Synthesis, characterization, in vitro antimicrobial, and anthelmintic evaluations of 2-(4-chloro-3-methylphenoxy)- N′-[{5′-(substituted aryl)-furan-2′-yl}-methylidene]-acetohydrazides.

Author

Varshney, Munendra, Husain, Asif, and Parcha, Versha

Abstract

In the present study, a novel series of 2-(4-chloro-3-methylphenoxy)- N′-[{5′-(substituted aryl)-furan-2′-yl}-methylidene]-acetohydrazides ( 4a- k) have been designed and synthesized with a new class of p-chloro- m-cresol Schiff bases, derived from the reaction of p-chloro- m-cresol 1, with ethylchloroacetate in anhydrous condition yielded 2-(4-chloro-3-methylphenoxy) acetate 2, which was treated with hydrazine hydrate to yield 2-(4-chloro-3-methylphenoxy) acetohydrazide 3, Further the resultant compound ( 3) was treated with different aromatic furfural aldehydes to yield Schiff bases ( 4a- k). All the synthesized compounds were confirmed to their spectral (IR, H NMR, C NMR, Mass, and CHN analysis) data. The current research also involved for their in vitro antibacterial screening in respect of the zone of inhibition (mm), against Gram-positive bacterial strains, Staphylococcus aureus (ATCC 11633), Bacillus cereus (ATCC 11778), Enterococcus faecalis (ATCC 14506), and Staphylococcus epidermidis (ATCC 155) and Gram-negative bacteria, Escherichia coli (ATCC10536), Salmonella typhi (MTCC 733), Shigella dysenteriae (ATCC 13313), and Klebsiella pneumoniae (ATCC 10031). Among the tested compounds, the most effective compound 4k exhibited very promising antibacterial activity when tested against strains of S. epidermidis, K. pneumoniae. While other compounds displayed moderate to good antibacterial activity. The synthesized Schiff bases also showed significant anthelmintic activity against two species of earthworms ( Pheretima posthuma and Perionyx excavates). [ABSTRACT FROM AUTHOR]

Published
2014
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40. Synthesis, biological activities, and pharmacokinetics studies of a mutual prodrug of aceclofenac and paracetamol.

Author

Husain, Asif, Ahuja, Priyanka, Shaharyar, M., Ahmad, Aftab, Mkhalid, Ibraheem, Alam, M., Akhter, M., and Zaman, M.

Abstract

An ester-based mutual prodrug (aceclofenac-paracetamol; AC-PR) was synthesized (one-pot method) with an aim of improving the therapeutic index through prevention of gastrointestinal irritation and bleeding that is associated with aceclofenac. The release of aceclofenac and paracetamol from the ester prodrug (AC-PR) was studied by reverse phase HPLC in hydrochloric acid buffer (pH 1.2), phosphate buffer (pH 7.4), 80 % v/v human plasma, 10 % w/v rat intestinal homogenate and 10 % w/v rat liver homogenate (pH 7.4). The prodrug showed negligible hydrolysis at pH 1.2 as compared to pH 7.4, suggesting that very less of the prodrug would hydrolyze in stomach, but would release the parent drugs at pH 7.4 in adequate amounts. The prodrug showed enhanced anti-inflammatory activity and significant protection against acetic acid-induced writhings (analgesic activity) as compared to that of aceclofenac. Further, the prodrug produced reduced number of ulcers as compared to that of the parent drug. These results suggest that the synthesized mutual prodrug (AC-PR) is better in terms of activity and GIT toxicity than the parent drug. [ABSTRACT FROM AUTHOR]

Published
2014
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41. Docking studies on butenolide derivatives as Cox-II inhibitors.

Author

Khokra, Sukhbir, Monga, Jyoti, Husain, Asif, Vij, Mohit, and Saini, Reetu

Abstract

To supplement hits from a high through put screening, a docking study on butenolides derivatives was performed as COX-II inhibitors. The fourteen ligands were docked inside the ligand-binding domain (LBD) of protein data bank PDB ID: 3HS5 utilizing Maestro version 9. Out of 14 compounds, compounds I and XII were found to embed in the hydrophobic pocket by forming hydrogen bonds with the amino acids HOH902, THR212, and THR206. Nitrogen of the pyrrolone ring of compound XII formed a strong hydrogen bond with THR206 with the distance of 2.221 Å and had showed highest glide score (−9.3) and lowest energy −95.66 kJ/mol. Glide score of Diclofenac and Celecoxib was found to be −10.33 and −11.37, respectively. Some other docked compounds also showed good glide scores comparable to standard anti-inflammatory drug Diclofenac, were III, V, VI, VII, IX, and XIV. Docking results were further validated by calculation of conformational energy, which was higher in case of Diclofenac and Celecoxib, i.e., −33.57 and −43.7 kJ/mol, respectively, in comparison to hypothetically designed compounds. The compounds that had highest glide score, lowest conformational energy are generally considered better and can be used for further drug designing and synthesize in laboratory. The most potent compound was XII having highest glide score and lowest conformational energy. [ABSTRACT FROM AUTHOR]

Published
2013
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42. Analytical methods for the detection of undeclared synthetic drugs in traditional herbal medicines as adulterants.

Author

Haneef, Jamshed, Shaharyar, Mohammad, Husain, Asif, Rashid, Mohd, Mishra, Ravinesh, Siddique, Nadeem A., and Pal, Manoj

Abstract

Traditional herbal medicines (THMs) are gaining popularity worldwide as an alternative approach to prescription drugs for many reasons including a general perception that they are safe. But recently there have been number of reported studies that reveal adulteration of THMs with undeclared synthetic drugs, which may potentially cause serious toxic adverse effects. This paper reviews the various classes of synthetic drugs that were found to be adulterated in THMs worldwide. The main focus is to highlight newer analytical tools used to detect adulteration. Due to the advancement in hyphenated techniques like liquid chromatography tandem mass spectrometry (LC-MS/MS), gas chromatography-tandem mass spectrometry (GC-MS/MS) and other conventional tools, it has become possible to detect synthetic drugs and their structural analogues as adulterants even if they are present in small quantities. This review also gives an overview of health-related risks after consuming such spurious products and challenges for future perspectives to control such type of malpractices. Copyright © 2013 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published
2013
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43. Design, synthesis and antihypertensive screening of novel pyridazine substituted s-triazin-2-imine/one/thione derivatives.

Author

Mishra, Ravinesh, Siddiqui, Anees A., Husain, Asif, Rashid, Mohd., and Goda, Chirag

Subjects
DRUG design, DRUG synthesis, ANTIHYPERTENSIVE agents, PYRIDAZINES, TRIAZINES, PYRIDAZINONES, DRUG standards
Abstract

Some new 7-substituted-phenyl-3,4,8,9-tetrahydro-2 H-pyridazino[1,6- a][1,3,5]triazin-2-imine/one/thione derivatives were synthesized by a sequence of reactions starting from appropriate aryl hydrocarbons. The final compounds were screened for antihypertensive activities by non-invasive method using Tail Cuff method. All the test compounds showed significant antihypertensive activity; 7-(biphenyl-4-yl)-3,4,8,9-tetrahydro-2 H-pyridazino[1,6- a][1,3,5]triazin-2-imine (4p) exhibited antihypertensive activity more than the reference standard drugs. [ABSTRACT FROM AUTHOR]

Published
2013
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45. Pharmacophore modeling studies on N-hydroxyphenyl acrylamides and N-hydroxypyridin-2-yl-acrylamides as inhibitor of human cancer leukemia K562 cells.

Author

Monga, Jyoti, Khokra, Sukhbir, and Husain, Asif

Abstract

In order to understand the essential structural features for inhibitors of human cancer leukemia K562 cells, three-dimensional pharmacophore hypotheses were built on the basis of a set of inhibitors of human cancer leukemia K562 selected from literature using PHASE program. Five point pharmacophore with two hydrogen bond acceptor (A), one hydrogen bond donor (D), and two aromatic rings (R) as pharmacophoric features were developed. Among them, the pharmacophore hypothesis AADRR 62 yielded a statistically significant 3D-QSAR model with as R value 0.883 and Q value 0.528 and was considered to be the best pharmacophore hypothesis. The developed pharmacophore model was externally validated by predicting the activity of test set molecules. The squared predictive correlation coefficient of 0.765 was observed between experimental and predicted activity values of test set molecules. [ABSTRACT FROM AUTHOR]

Published
2013
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46. Synthesis and antimicrobial activity of bischalcone derivatives.

Author

Husain, Asif, Ahmad, Aftab, Mkhalid, Ibraheem, Mishra, Ravinesh, and Rashid, Mohd

Abstract

Several bischalcones ( 2a- h and 5a- e) and flavones ( 3a- f) were synthesized and evaluated for their antimicrobial actions. Bischalcones were prepared by condensing 1,1′-(4,6-dimethyl-1,3-phenylene)diethanone ( 1) or 1-(5-acetyl-2,4-dimethoxyphenyl)-1-ethanone ( 4) with arylaldehydes. Bischalcones were cyclized in presence of iodine to give corresponding flavones ( 3a- f). An alternative route to synthesize the flavones consisted in preparing the diester derivatives ( 6a- f) of ( 1) with different aromatic acids, which could be converted to β-diketones followed by cyclization to give the corresponding flavones. However, all the attempts in this direction were unsuccessful and it could not be possible to proceed beyond diester stage; six diester derivatives ( 6a- f) were synthesized. The structures of the synthesized compounds were assigned on the basis of H NMR, mass spectral data and microanalyses results. The antimicrobial screening was performed at a concentration of 100 μg/mL by cup plate method; the compounds inhibiting growth of one or more of the microorganisms were further tested for their minimum inhibitory concentration (MIC) by turbidity method. Preliminary antimicrobial results revealed that the compounds 2a- h and 3a- f were significant in their antibacterial and antifungal activities. MICs results showed that the compound 2f exhibited very good activity against E. coli, P. aeruginosa, and C. albicans with MIC-12.5 μg/mL. Similar type of activity was shown the compound 3a against S. aureus and C. albicans with MIC-12.5 μg/mL. Another compound, 3f, was active against P. aeruginosa and C. albicans with MIC-12.5 μg/mL. Methylation of the two chelated hydroxyls ( 5a- e) significantly reduced the activity. However, oxidative cyclization of bischalcones resulted in compounds ( 3a- f) which were found to be considerably active. Diesters ( 6a- f) were insignificant in their antimicrobial activities. [ABSTRACT FROM AUTHOR]

Published
2013
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47. Synthesis and biological evaluation of di- and tri-substituted imidazoles as safer anti-inflammatory-antifungal agents.

Author

Husain, Asif, Drabu, Sushma, Kumar, Nitin, Alam, M. M., and Bawa, Sandhya

Subjects
IMIDAZOLES, ANTIFUNGAL agents, NONSTEROIDAL anti-inflammatory agents, NUCLEAR magnetic resonance, PHYSIOLOGICAL effects of analgesics, POLYPHARMACY
Abstract

PURPOSE: In view of the potential pharmacophoric nature of imidazole nucleus, two series of imidazole derivatives, 2,4‑disubstituted‑1 H‑imidazoles (2a‑m) and 1,2,4‑trisubstituted‑1 H‑imidazoles (3a‑m), were synthesized with an aim of obtaining dual acting compounds i.e., anti‑inflammatory and antifungal agents. MATERIALS AND METHODS: The title compounds were synthesized from 4‑methoxyphenyl glyoxal (1) following multistep synthesis, and their structures were established on the basis of modern analytical techniques (IR, NMR and MS). The synthesized imidazoles were tested for their in vivo anti‑inflammatory activity. In addition to that, some compounds were also evaluated for their analgesic and ulcerogenic effects. The compounds were also evaluated for their in vitro antifungal activity. RESULTS: Di‑ and tri‑substituted imidazole derivatives (2a‑m and 3a‑m) were successfully synthesized. In in vivo anti‑inflammatory test, six compounds (2 h, 2 l, 3 g, 3 h, 3 l and 3 m) exhibited good anti‑inflammatory activity (49.58 to 58.02% inhibition) with minimal GI irritation (severity index; 0.17 to 0.34). These compounds were also tested for their analgesic activity and showed appreciable protection (40.53 to 49.60% protection) against saline‑induced writhing test. Indomethacin was used as standard drug for comparison. In antifungal test, two compounds (3 h and 3 l) displayed appreciable antifungal activity (MIC; 12.5 μg mL‑1) against the fungal strains tested. CONCLUSION: Two compounds, 2‑(4‑nitrophenyl)‑4‑(4‑methoxyphenyl)‑1‑phenyl‑1H‑imidazole (3 h) and 2,4‑di‑(4‑methoxyphenyl)‑1‑phenyl‑1H‑imidazole (3 l), emerged as lead compounds having dual biological activities; good anti‑inflammatory as well as antifungal effect with lesser GI irritation. [ABSTRACT FROM AUTHOR]

Published
2013
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48. Quinolone derivatives as antitubercular drugs.

Author

Asif, Mohammad, Siddiqui, Anees, and Husain, Asif

Abstract

New chemotherapeutic drugs are the need to improve tuberculosis (TB) control particularly due to the emergence of multidrug-resistant strains and extensively drug-resistant strains of TB. These antitubercular compounds have different chemical moieties in their structure. Quinolones are generally used against many Gram-positive and Gram-negative bacteria. They are also active against atypical mycobacteria. Some quinolones (ciprofloxacin, levofloxacin, etc.) inhibit strains of Mycobacterium tuberculosis at concentrations <2.0 μg/mL. Fluoroquinolones are an important recent addition to the drugs available for TB, especially for strains that are resistant to first-line agents. The present review provides an overview of the drugs that are being used have quinolone moieties in TB treatment. [ABSTRACT FROM AUTHOR]

Published
2013
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49. Heterocyclic compounds as carbonic anhydrase inhibitor.

Author

Husain, Asif and Madhesia, Diwakar

Subjects
DRUG design, HETEROCYCLIC compounds, CARBONIC anhydrase inhibitors, TARGETED drug delivery, BIOSYNTHESIS, SULFONAMIDE drugs, NEUROMUSCULAR diseases, GLAUCOMA treatment
Abstract

The carbonic anhydrases (CAs, EC 4.2.1.1) constitute interesting targets for the design of pharmacological agents useful in the treatment or prevention of a variety of disorders such as, glaucoma, acid-base disequilibria, epilepsy, and other neuromuscular diseases, altitude sickness, edema, and obesity. A quite new and unexpected application of the CA inhibitors (CAIs) is with regard to their potential use in the management (imaging and treatment) of hypoxic tumors. A series of sulfonamides, including some clinically used derivatives like acetazolamide, methazolamide, ethoxzolamide, dichlorophenamide, dorzolamide, brinzolamide, benzolamide, and sulpiride, or indisulam, a compound in clinical development as antitumor drug, as well as the sulfamate antiepileptic drug topiramate have been reported to inhibit various human carbonic anhydrase isozyme. Various heterocyclic sulfonamides have been reported in this review with their potency to inhibit different carbonic anhydrases isozymes. [ABSTRACT FROM AUTHOR]

Published
2012
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50. 1-(1H-Benzimidazol-2-yl)-3-[5-(trichloromethyl)-1,3,4-oxadiazol-2-yl]propan-1-one.

Author

Rashid, Mohd, Husain, Asif, Mishra, Ravinesh, Ahmed, Niyaz, and Siddique, Nadeem Ahmed

Subjects
BENZIMIDAZOLES, OXADIAZOLES, PROPANE, MICROWAVES, ACETIC acid, NUCLEAR magnetic resonance spectroscopy, HYDRAZIDES
Abstract

The title compound, 1-(1H-benzimidazol-2-yl)-3-[5-(trichloromethyl)-1,3,4-oxadiazol-2-yl]propan-1-one (2) was synthesized successfully from 4-(1H-benzimidazol-2-yl)-4-oxobutanehydrazide (1) under microwave irradiation in good yield by reacting with trichloroacetic acid, and the structure of title compound was confirmed on the basis of IR, 1H-NMR, 13C-NMR, MS and CHN analyses results. [ABSTRACT FROM AUTHOR]

Published
2012
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