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Complexes of Ruthenium and Osmium Based on Oxicam Scaffold As Potential Anticancer Agents

Thesis Info

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Author

Ashraf, Adnan

Program

PhD

Institute

University of Sargodha

City

Sargodha

Province

Punjab

Country

Pakistan

Thesis Completing Year

2017

Thesis Completion Status

Completed

Subject

Chemistry

Language

English

Link

http://prr.hec.gov.pk/jspui/bitstream/123456789/11301/1/Adnan%20Ashraf_Chem_2017_UoSargodha_PRR.pdf

Added

2021-02-17 19:49:13

Modified

2024-03-24 20:25:49

ARI ID

1676725775468

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Metal based drugs have been used for medicinal purposes since ages but their potential was realized after the discovery of the first metal based chemotherapeutic agent, i.e., cisplatin, which became one of the most successful anticancer drugs espcecially for the treatment of testicular cancer. Other members of this class include oxaliplatin, carboplatin and nedaplatin. The use of platinum based drugs is limited due to their adverse side effects (e.g., nephrotoxicity, neurotoxicity, nausea, vomiting etc.) and intrinsic or acquired resistance. These limitations prompted bioinorganic chemists to develop new strategies to treat cancer with other metal based anticancer agents with higher efficacy and lesser undesired effects. Therefore, different metal complexes of titanium, iron, cobalt, gallium, ruthenium and osmium etc. were investigated. Among these NAMI-A (imidazolium [tetrachlorido(dimethylsulfoxide)(1Himidazole)ruthenate(III)]), KP46 (trismaltolate gallium) and KP1019 (indazolium trans[tetrachloridobis(1H-indazole)ruthenate(III)]) have enteredclinical trials. On the other hand, Ru(II)/Os(II) half sandwich organometallic complexes increase the lipophilic character of complexes and facilitate their uptake into cells. RAPTA type complexes are among the most popular examples of half sandwich organometallics. Furthermore, the coordination of bioactive ligands with these established organometallic pharmacophores may enhance the efficacy of these biologically active compounds by altering their physicochemical and pharmacological properties. In particular, the use of bioactive ligands such as hydroxypyrones, quinolones and non-steroidal anti-inflammatory drugs (NSAIDs) often resulted in promising bioactivity of the compounds. In this thesis, the use of oxicam based NSAIDS as ligands for Ru(II) and Os(II) was investigated. For this purpose different series of ligands based on the oxicam scaffold were prepared. These include 1,2-benzothiazine based primary amides, secondary amides, indazole and methyl pyridyl based secondary amides, piroxicam as well as isoxicam analogues, 1,2-benzothiazine based α,βunsatuarated ketones and pyrazole based benzenesulfonamides. Furthermore, these ligands were reacted with Ru(II) and Os(II) cymene dimer to obtain organometallic complexes. All the ligands and complexes were characterized with different spectroscopic techniques including FT-IR, 1H, 13C NMR, elemental analysis, high resolution mass spectrometry and twenty seven compounds were analyzed by single crystal X-ray diffraction analysis. The cytotoxic activity of the complexes towards human colorectal carcinoma HCT116, non-small cell lung carcinoma NCIH460 and cervical carcinoma SiHa cells was investigated by using the sulforhodamine B (SRB) assay. The prepared ligands behaved as monodentate (N donor) or bidentate chelators (O,O-, N,O- and N,N-donor systems) depending upon the ligand structure as well as reaction conditions such as xxix nature of solvent used for reaction. The 1,2-benzothiazine based primary amides were synthesized by reacting compound 5 with different alkylating agents in basic conditions to isolate ligands 6a-g. These O,O-coordinating ligands were used to synthesize the organometallic ruthenium complexes 7a-g (Scheme-1) with piano-stool configuration. These complexes were evaluated for their anticancer activity and results indicate that only 7f and 7g were active against three different human cancer cell lines. On the other hand, 1,2-benzothiazine based secondary amides were synthesized by reacting compound 8 with different aniline derivatives to obtain O,O-chelating ligands 9a-g. When these ligands were reacted with [Ru(cym)Cl2]2, the same O,Ocoordination behavior was observed to stabilize metal complexes 10a-g by forming sixmembered rings and giving rise to piano stool type geometry (Scheme-2). All these complexes were found active against different anticancer cell lines and the most lipophilic compound was found the most active with an IC50 value of 13.58 µM. The N-benzyl analogues of piroxicam and isoxicam 11 and 12 were also prepared and reacted with MII(η6-p-cymene). Compounds 11 and 12 can act as monodentate ligands through their pyridyl/isoxazolyl nitrogen atom and as bidentate chelators to Ru(II) and Os(II) metal ions by forming six membered rings through pyridyl/isoxazolyl nitrogen and the amide oxygen atoms (Scheme-3). In compounds 15-18 functionalization at position 3 was carried out to get indazolyl/pyridyl goup-containing oxicam analogues which act as monodentate ligands and coordinate to ruthenium/osmium centres through pyridyl/indazolyl nitrogens. The results of anticancer activity studies revealed that organo-Ru(II) and -Os(II) complexes 18a-c are more active than the free ligand 18 (Scheme-4). The 1,2-benzothiazine based chalcones (Scheme-5) were obtained as intermediates which were reacted with hydrazine to isolate 1,2-benzothiazine based pyrazole containing sulphonamide ligands 21a-j. The results of anticancer activity assays show that halogen containing derivatives are more active in this series (Scheme-6). These pyrazole containing sulphonamides were reacted with [Ru(cym)Cl2]2 to isolate complexes in which these sulfonamides acted either asmonodentate or bidentate ligands. In complexes 22a-k ligands coordinated mondentately through the pyrazole nitrogen (Scheme-7) while in complexes 23a-g they coordinated bidentately via pyrazole and sulphonamide nitrogen atoms by forming rather stable seven membered rings (Scheme-8). The biological investigations indicate moderate to high IC50 values for these complexes and it was also observed that within the series of compounds, the most lipophilic complex was the most active.
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گُن اُنؐ کے ہی گاتا ہے اپنا کہ بیگانہ ہے


گُن اُنؐ کے ہی گاتا ہے اپنا کہ بیگانہ ہے
’’اِک میں ہی نہیں اُن پر قربان زمانہ ہے‘‘

حامدؐ بھی وہ احمدؐ بھی ‘ محمودؐ و محمد ﷺ بھی
’’جو ربِ دو عالم کا محبوب یگانہ ہے‘‘

صد کیف کا عالم ہے اِک پل تیری مدحت کا
صد رشکِ گہر اُس پل آنکھوں کا بھر آنا ہے

بچپن سے ہی ہونٹوں پر سرکارؐ کی مدحت ہے
ٹوٹے نہ الٰہی یہ بندھن جو پُرانا ہے

جس ذاتؐ کی آمد پر کعبے پہ لگا جھنڈا
اُس ذاتؐ کی آمد پر راہوں کو سجانا ہے

مدحِ شہِؐ خوباں سے عرفاںؔ کی زباں تر ہے
شاہوں کے قصائد نہ گفتارِ زمانہ ہے

سائیں رفیق رانجھا تے بابا جی قصور مند

This article covers the poetic and research services of Sufi poet Sain Muhammad Rafique Ranjha from Hamza Ghous Sialkot. He is a Punjabi "Sofi "poet and a compiler. In this article, I have already mentioned his own poetry collection and life. In his own book, he has used a dozen genres of poetry. This Sufi poet, who is experimenting with new and old genres, but “Rubai” is his favorite genre. The first book "Warasat-e- Faqr" by Sain Muhammad Rafique Ranja consists of 418 pages which has been composed. While the second book “Suchay Moti” is by the famous Punjabi poet of Gujarat Baba Ji Qasoor Mand which has 290 pages. It is published in 2017. Both books contain mystical poetry. Along with the books, brief information about the lives of the authors is also given.

Association Mapping for Drought Tolerance in Wheat Triticum Aestivum L.

Fluctuating climatic conditions and increasing dearth of water resources are severely affecting crop yields. The present study was conducted to explore the genetic diversity for drought tolerance in bread wheat (Triticum aestivum L.) which can be used in future breeding programs. For this purpose, 200 genotypes of bread wheat (Triticum aestivum L.) comprising current cultivars, land races and improved lines were phenotyped over two consecutive seasons (2009-2010 and 2010-2011). Analysis of variance showed significant variation in several morphological and physiological traits including peduncle length (PL), extrusion length (EL), awn length (AL), plant height (PH), leaf rolling (LR), waxiness (WAX), relative water content (RWC), accumulation of proline (Pro), seed size (SZ), grains per spike (gr/sp) and yield/plant (Y) under normal and drought conditions during both years. Using multivariate analysis, two data sets C&S (control and stressed) and C-S/C (relative performance) were prepared to examine plant responses to drought stress. 1st principle component (PC) accounted 24.97% variation for the 1st year and 43.85% variation for the 2nd in C&S dataset. For C-S/C dataset, 18.12% and 15.58% variation was observed in the 1st and 2nd years, respectively. For association mapping, 108 diverse wheat accessions were selected to tag molecular markers for drought tolerance using 25 SSR loci located on chromosome 2A. To eliminate spurious associations, population structure and kinship were taken into account using 30 unlinked markers covering all 21 chromosomes. A total of 11 markers were found associated using MLM (mixed linear model) approach with phenotypic variability ranging from 6.56 to 17.8%. The marker wmc455 was found associated with seed size (r2 7.6%) and plant height (r2 7.3%) under drought conditions. The relative water content was found associated with gwm312 under drought conditions for both years’ data. The marker barc124 showed association with three different traits under different treatments. The study detected novel QTLs for drought adaptive traits and can be used for marker assisted breeding to enhance wheat performance under drought conditions.