Sathyamangalam V. Balasubramanian scite author profile

Lipopolysaccharide (LPS), the major cell wall constituent of Gram-negative bacteria, evokes a multitude of biological effects in mammals including pyrogenicity and toxic shock syndrome. Polymyxin B (PmB), a polycationic cyclic peptide, is known to neutralize most of its activities. The nature of the interaction of PmB with LPS and lipid A was investigated by isothermal titration calorimetry. PmB binds to LPS as well as lipid A stoichiometrically and non-co-operatively with micromolar affinity. These interactions are driven primarily by a favourable change in entropy (delta S) and are endothermic in nature. These positive changes in enthalpies decrease with increasing temperature, yielding a heat capacity change, delta Cp, of -2385 J.mol-1.degree-1 for PmB-LPS interactions while the binding of PmB to lipid A displays a delta Cp of -2259 J.mol-1.degree-1. The negative heat capacity changes provide strong evidence for the role of hydrophobic interactions as the driving force for the association of PmB with LPS and lipid A. A correlation of the energetics of these interactions with analyses of the molecular models of PmB suggests that a cluster of solvent-exposed non-polar amino acid side-chains that line one surface of the molecule, together with a ring of positively charged residues on its other surface, are responsible for its strong and stoichiometric binding to LPS.

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Taxol-Lipid Interactions: Taxol-Dependent Effects on the Physical Properties of Model Membranes

Balasubramanian

Straubinger²

1994

Biochemistry

114

101

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Taxol (paclitaxel) is a diterpenoid anticancer agent undergoing intensive human clinical evaluation. The poor aqueous solubility of taxol necessitates administration in excipients causing a variety of adverse effects, including anaphylactoid hypersensitivity reactions. Recently, taxol has been formulated in better-tolerated drug carriers such as liposomes. We investigated the conformation of taxol and the interaction of taxol with dipalmitoylphosphatidylcholine (DPPC) liposomes using fluorescence, circular dichroism, differential scanning calorimetry, fluorescence polarization, and X-ray diffraction. The conformation of taxol in DPPC membranes was similar to that observed in nonpolar solvents such as chloroform. Taxol was found to partition into the bilayer, perturbing the hydrocarbon chain conformation. The taxol C13 side chain was found to be fluorescent, and it displays an environment-sensitive shift in emission spectrum; taxol fluorescence was used to confirm the insertion of the drug into the bilayer. Taxol induces a broadening of the DPPC phase transition, and the location of the drug in the bilayer depends on drug concentration. Incorporation of taxol affects other physical properties of the bilayer such as the lipid order parameter, and this fluidizing effect was also observed upon incorporation of taxol in biological membranes isolated from basolateral plasma membranes of rat liver. These studies demonstrate that taxol incorporated into liposomes penetrates into the acyl chain domain of the bilayer and alters the physical properties of both artificial and biological membranes.

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Influence of aggregation on immunogenicity of recombinant human Factor VIII in hemophilia A mice

Purohit

Middaugh

Balasubramanian

2006

Journal of Pharmaceutical Sciences

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Recombinant human factor VIII (rFVIII), a multidomain glycoprotein is used in replacement therapy for treatment of hemophilia A. Unfortunately, 15%-30% of the treated patients develop inhibitory antibodies. The pathogenesis of antibody development is not completely understood. The presence of aggregated protein in formulations is generally believed to enhance the immune response. rFVIII has a tendency to aggregate but the effect of such aggregation on the immunogenicity of rFVIII is not known. We have, therefore, characterized aggregated rFVIII produced by thermal stress and evaluated its effect on the immunogenicity of rFVIII in hemophilia A mice. Aggregated rFVIII alone and mixtures of rFVIII with aggregated rFVIII were less immunogenic than native rFVIII. In vitro Th-cell proliferation studies and cytokine analyses conducted on splenocytes obtained from immunized animals suggest that aggregated rFVIII behaves as a unique antigen compared to native monomeric rFVIII. The antigenic properties of the aggregated and native rFVIII were compared using ELISAs (epitope availability) and cathepsin-B (an antigen processing enzyme) digestion. The data suggest significant differences in the antigenic properties of rFVIII and aggregated rFVIII. Overall it appears that aggregated rFVIII does not enhance the immunogenicity (inhibitor development) of rFVIII in hemophilia A mice but rather acts as a distinct antigen.

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Influence of cationic lipids on the stability and membrane properties of paclitaxel‐containing liposomes

Campbell

Balasubramanian

Straubinger

2001

Journal of Pharmaceutical Sciences

117

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Pharmaceutical and Physical Properties of Paclitaxel (Taxol †) Complexes with Cyclodextrins ‡

Sharma

Balasubramanian

Straubinger

1995

Journal of Pharmaceutical Sciences

160

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Lower Inhibitor Development in Hemophilia A Mice following Administration of Recombinant Factor VIII-O-Phospho-L-serine Complex

Purohit

Ramani

Sarkar

et al. 2005

Journal of Biological Chemistry

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Factor VIII is a multidomain protein composed of A1, A2, B, A3, C1, and C2 domains. Deficiency or dysfunction of factor VIII causes hemophilia A, a bleeding disorder. Administration of exogenous recombinant factor VIII as a replacement leads to development of inhibitory antibodies against factor VIII in 15-30% of hemophilia A patients. Hence, less immunogenic preparations of factor VIII are highly desirable. Inhibitory antibodies against factor VIII are mainly directed against immunodominant epitopes in C2, A3, and A2 domains.

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Phospholipid-cationic lipid interactions: influences on membrane and vesicle properties

Campbell

Balasubramanian

Straubinger

2001

Biochimica et Biophysica Acta (BBA) - Biomembranes

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Liposomes composed of synthetic dialkyl cationic lipids and zwitterionic phospholipids such as dioleoylphosphatidylethanolamine have been studied extensively as vehicles for gene delivery, but the broader potentials of these cationic liposomes for drug delivery have not. An understanding of phospholipid-cationic lipid interactions is essential for rational development of this potential. We evaluated the effect of the cationic lipid DOTAP (N-[1-(2,3-dioleoyloxy)propyl]-N,N,N-trimethylammonium) on liposome physical properties such as size and membrane domain structure. DSC (differential scanning calorimetry) showed progressive decrease and broadening of the phase transition temperature of dipalmitoylphosphatidylcholine (DPPC) with increasing fraction of DOTAP, in the range of 0.4-20 mol%. Laurdan (6-dodecanolyldimethylamino-naphthalene), a fluorescent probe of membrane domain structure, showed that DOTAP and DPPC remained miscible at all ratios tested. DOTAP reduced the size of spontaneously-forming PC-containing liposomes, regardless of the acyl chain length and degree of saturation. The anionic lipid DOPG (dioleoylphosphatidylglycerol) had similar effects on DPPC membrane fluidity and size. However, DOTAP/DOPC (50/50) vesicles were taken up avidly by OVCAR-3 human ovarian tumor cells, in contrast to DOPG/DOPC (50/50) liposomes. Overall, DOTAP exerts potent effects on bilayer physical properties, and may provide advantages for drug delivery.

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Solvent- and Concentration-Dependent Molecular Interactions of Taxol (Paclitaxel †)

Balasubramanian

Alderfer

Straubinger

1994

Journal of Pharmaceutical Sciences

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