Suresh K. Bhargava

Unprecedented near-infrared (NIR) emission in diplatinum(III) (d7-d7) complexes at room temperature.

The synthesis and single-crystal X-ray structures of the first family of efficient NIR emitters with tunable emission energy based on dihalodiplatinum(III) (5d(7)-5d(7)) complexes of general formulae [Pt(2)(mu-C(6)H(3)-5-R-2-AsPh(2))(4)X(2)] (R = Me or CHMe(2); X = Cl, Br or I), together with that of their diplatinum(II) (5d(8)-5d(8)) precursors ([Pt(2)(mu-C(6)H(3)-5-R-2-AsPh(2))(4)]) and cyano counterparts (X = CN), are reported. The diplatinum(II) complexes with isopropyl groups are isolated initially as a mixture of two species, one being a half-lantern structure containing two bridging and two chelate C(6)H(3)-5-CHMe(2)-2-AsPh(2) ligands (1b) that exists in two crystalline modifications [d(Pt...Pt) = 3.4298(2) A and 4.3843(2) A]; the other is a full-lantern or paddle-wheel structure having four bridging C(6)H(3)-5-CHMe(2)-2-AsPh(2) ligands (2b) [d(Pt...Pt) = 2.94795(12) A]. Complete conversion of the isomers into 2b occurs in hot toluene. The Pt-Pt bond distances in the diplatinum(III) complexes are less than that in 2b and increase in the order X = Cl (3b) [2.6896(2) A] < Br (4b) [2.7526(3) A] < I (5b) [2.7927(7) A] approximately CN (6b) [2.7823(2), 2.7924(2) A for two independent molecules]. Comparison with the corresponding data for our previously reported series of complexes 3a-6a (R = Me) indicates that the Pt-Pt bond lengths obtained from single-crystal X-ray analysis are influenced both by the axial ligand and by intermolecular lattice effects. Like [Pt(2)(mu-pop)(4)](4-) [pop = pyrophosphite, (P(2)O(5)H(2))(2-)], the diplatinum(II) complexes [Pt(2)(mu-C(6)H(3)-5-R-2-AsPh(2))(4)] [R = Me (2a), CHMe(2) (2b)] display intense green phosphorescence, both as solids and in solution, and at room temperature and 77 K, with the emission maxima in the range 501-532 nm. In contrast to the reported dihalodiplatinum(III) complexes [Pt(2)(mu-pop)(4)X(2)](4-) that exhibit red luminescence only at 77 K in a glass or as a solid, complexes 3a-6a and 3b-6b are phosphorescent in the visible to near-infrared region at both room and low temperatures. The electronic spectra and photoemissive behavior are discussed on the basis of time-dependent density functional theory (TDDFT) calculations at the B3YLP level. The photoemissive states for the halide analogues 3a,b-5a,b involve a moderate to extensive mixing of XMMCT character and MC [d sigma-d sigma*] character, whereas the cyano complexes 6a and 6b are thought to involve relatively less mixing of the XMMCT character into the MC [d sigma-d sigma*] state.

High surface area Au–SBA-15 and Au–MCM-41 materials synthesis: Tryptophan amino acid mediated confinement of gold nanostructures within the mesoporous silica pore walls

Advantages of confining the gold nanostructures formation within the mesoporous silica pore walls during its silica condensation and consequent improvement in the textural properties such as specific surface area, pore volume, pore diameter have been demonstrated, while retaining gold nanostructures within the silica walls. This has been achieved by tryptophan mediated confinement of gold nanoparticles formation within the condensing silica framework, to obtain Au-SBA-15 (SSA 1247 m(2)/g, V(t)~1.37 cm(3)/g) and Au-MCM-41 (SSA 1287 m(2)/g, V(t)~1.1 cm(3)/g), mesoporous silica materials having the combination of very high surface area from the porous support as well as gold nanoparticles infiltrated silica walls. Choice of tryptophan for this purpose is that it has an indole group, which was known to reduce gold ions to form gold nanoparticles and its amine and carboxylic acid groups, catalyze the hydrolysis of silica precursors in a wide range of pH. These properties have been utilized in restricting the gold nanostructures formation inside the condensing silica phase without affecting the self assembly between the silica precursors and the triblock copolymer (for SBA-15) or cetyltrimethylammonium bromide template (for MCM-41). The polytryptophan and the gold nanostructures, which were encapsulated within the silica framework and upon removal of the template by calcination resulting in the formation mesoporous materials wherein the silica walls become microporous due to the removal of occluded polytryptophan and the resulting microchannels contain very small gold nanostructures. Hence, the resulting materials have very high surface area, high pore volume and narrow pore size distribution as compared to their parent SBA-15, MCM-41 and SBA-15, MCM-41 post functionalized with gold nanoparticles inside the pores.

Synthesis of 2,3,6,7-tetramethoxyphenanthren-9-amine: An efficient precursor to access new 4-aza-2,3-dihydropyridophenanthrenes as apoptosis inducing agents

A new route for the synthesis of novel 2,3,6,7-tetramethoxy phenanthrene amine precursor has been successfully accomplished. Subsequently, this amine precursor has been directly utilized for the synthesis of a new series of 4-aza-2,3-dihydropyridophenanthrene derivatives via a three component reaction with tetronic acid and substituted aldehydes. These compounds were evaluated for their cytotoxic potential against human lung (A549), prostate (PC-3 and DU145), breast (MDA-MB-231 and 4T1), gastric (HGC-27), colon (Caco-2) and cervical (HeLa) cancer cell lines. Compound 10l showed significant anticancer profile against DU145xa0cell line with an IC50 value of 2.6xa0±xa00.34xa0μM. Disruption of F-actin cytoskeleton structure and cell migration inhibition in DU145xa0cells clearly indicate that the tumor progression and metastasis are affected by this compound (10l). Cell cycle analysis revealed that it arrests the cells in G2/M phase. Acridine orange/ethidium bromide (AO/EB) staining, Hoechst staining and annexin-V binding assays showed that cell proliferation is inhibited through induction of apoptosis. Moreover, its treatment leads to collapse of the mitochondrial membrane potential (DΨm).

Self-Assembled Functional Nanostructure of Plasmid DNA with Ionic Liquid [Bmim][PF6]: Enhanced Efficiency in Bacterial Gene Transformation

The electrostatic interaction between the negatively charged phosphate groups of plasmid DNA and the cationic part of hydrophobic ionic liquid 1-butyl-3-methylimidazolium hexafluorophosphate ([Bmim][PF6]), initiates spontaneous self-assembly to form the functional nanostructures made up of DNA and ionic liquid (IL). These functional nanostructures were demonstrated as promising synthetic nonviral vectors for the efficient bacterial pGFP gene transformation in cells. In particular, the functional nanostructures that were made up of 1 μL of IL ([Bmim][PF6]) and 1 μg of plasmid DNA can increase the transformation efficiency by 300-400% in microbial systems, without showing any toxicity for E. coli DH5α cells. (31)P nuclear magnetic resonance (NMR), Fourier transform infrared (FTIR) spectroscopy, and X-ray photoelectron (XPS) spectroscopic analysis revealed that the electrostatic interaction between negatively charged phosphate oxygen and cationic Bmim(+) tends to initiate the self-assembly process. Thermogravimetric analysis of the DNA-IL functional nanostructures showed that these nanostructures consist of ∼16 wt % ionic liquid, which is considered to provide the stability to the plasmid DNA that eventually enhanced the transformation efficiency.

Anti-cancer gold(I) phosphine complexes: Cyclic trimers and tetramers containing the P-Au-P moiety

We report the application of cationic tri- and tetra-nuclear gold(I) phosphine complexes [Au3(μ-dppen)3]X3 and [Au4(μ-dppa)4]X4 (X=OTf, PF6) [OTf=trifluoromethanesulfonate, dppen=trans-1,2-bis(diphenylphosphino)ethene, dppa=bis(diphenylphosphino)acetylene] for cancer treatment. The results of cytotoxicity tests on four different cancer cells [prostate (DU145), cervical (HeLa), breast (MDAMB-231) and fibro sarcoma (HT1080)] indicate these complexes possess remarkable tumor cell growth inhibitory effects and high selectivity towards cancer cells. The anti-tumor mechanism of the tri- and tetra-nuclear gold(I) complexes has also been investigated.

Synthesis of gold(I) phosphine complexes containing the 2-BrC6F4PPh2 ligand: Evaluation of anticancer activity in 2D and 3D spheroidal models of HeLa cancer cells

Newly synthesised mononuclear gold complexes containing the 2-BrC6F4PPh2 ligand have been fully characterised and their anticancer activity towards five human tumor [prostate (PC3), glioblastoma (U87MG), cervical (HeLa), fibrosarcoma (HT1080), ovarian (SKOV-3)] and normal human embryonic kidney (Hek-293T) cell lines investigated. Some of the synthesised gold complexes displayed higher cytotoxicity than cisplatin towards PC-3, HeLa and U87MG cells and inhibited the thioredoxin reductase (TrxR) enzyme, which is considered a potential target for new compounds in cancer treatment. The more physiologically relevant tumor spheroid assay demonstrated the superior potency of these gold phosphine complexes in inhibiting the growth of cervical carcinoma cell line HeLa (3D) spheroidal models. The mechanism of cell death was shown to be apoptotic cell death through cell cycle arrest, mitochondrial membrane depolarisation and increased ROS production.