Thilani N. Samarakoon
Kansas State University
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Featured researches published by Thilani N. Samarakoon.
BMC Cancer | 2010
Sivasai Balivada; Raja Shekar Rachakatla; Hongwang Wang; Thilani N. Samarakoon; Raj Kumar Dani; Marla Pyle; Franklin Orban Kroh; Brandon Walker; Xiaoxuan Leaym; Olga Koper; Masaaki Tamura; Viktor Chikan; Stefan H. Bossmann; Deryl L. Troyer
BackgroundThere is renewed interest in magnetic hyperthermia as a treatment modality for cancer, especially when it is combined with other more traditional therapeutic approaches, such as the co-delivery of anticancer drugs or photodynamic therapy.MethodsThe influence of bimagnetic nanoparticles (MNPs) combined with short external alternating magnetic field (AMF) exposure on the growth of subcutaneous mouse melanomas (B16-F10) was evaluated. Bimagnetic Fe/Fe3O4 core/shell nanoparticles were designed for cancer targeting after intratumoral or intravenous administration. Their inorganic center was protected against rapid biocorrosion by organic dopamine-oligoethylene glycol ligands. TCPP (4-tetracarboxyphenyl porphyrin) units were attached to the dopamine-oligoethylene glycol ligands.ResultsThe magnetic hyperthermia results obtained after intratumoral injection indicated that micromolar concentrations of iron given within the modified core-shell Fe/Fe3O4 nanoparticles caused a significant anti-tumor effect on murine B16-F10 melanoma with three short 10-minute AMF exposures. We also observed a decrease in tumor size after intravenous administration of the MNPs followed by three consecutive days of AMF exposure 24 hrs after the MNPs injection.ConclusionsThese results indicate that intratumoral administration of surface modified MNPs can attenuate mouse melanoma after AMF exposure. Moreover, we have found that after intravenous administration of micromolar concentrations, these MNPs are capable of causing an anti-tumor effect in a mouse melanoma model after only a short AMF exposure time. This is a clear improvement to state of the art.
ACS Nano | 2010
Raja Shekar Rachakatla; Sivasai Balivada; Gwi-Moon Seo; Carl Myers; Hongwang Wang; Thilani N. Samarakoon; Raj Kumar Dani; Marla Pyle; Franklin Orban Kroh; Brandon Walker; Xiaoxuan Leaym; Olga Koper; Viktor Chikan; Stefan H. Bossmann; Masaaki Tamura; Deryl L. Troyer
Localized magnetic hyperthermia as a treatment modality for cancer has generated renewed interest, particularly if it can be targeted to the tumor site. We examined whether tumor-tropic neural progenitor cells (NPCs) could be utilized as cell delivery vehicles for achieving preferential accumulation of core/shell iron/iron oxide magnetic nanoparticles (MNPs) within a mouse model of melanoma. We developed aminosiloxane-porphyrin functionalized MNPs, evaluated cell viability and loading efficiency, and transplanted neural progenitor cells loaded with this cargo into mice with melanoma. NPCs were efficiently loaded with core/shell Fe/Fe(3)O(4) MNPs with minimal cytotoxicity; the MNPs accumulated as aggregates in the cytosol. The NPCs loaded with MNPs could travel to subcutaneous melanomas, and after A/C (alternating current) magnetic field (AMF) exposure, the targeted delivery of MNPs by the cells resulted in a measurable regression of the tumors. The tumor attenuation was significant (p < 0.05) a short time (24 h) after the last of three AMF exposures.
Methods of Molecular Biology | 2012
Thilani N. Samarakoon; Sunitha Shiva; Kaleb Lowe; Pamela Tamura; Mary R. Roth; Ruth Welti
Herein, current approaches to electrospray ionization mass spectrometry-based analyses of membrane lipid molecular species found in Arabidopsis thaliana are summarized. Additionally, the identities of over 500 reported membrane lipid molecular species are assembled.
ChemBioChem | 2015
Cindy Y. Jao; Daniel Nedelcu; Lyle V. Lopez; Thilani N. Samarakoon; Ruth Welti; Adrian Salic
Cholesterol is a fundamental lipid component of eukaryotic membranes and a precursor of potent signaling molecules, such as oxysterols and steroid hormones. Cholesterol and oxysterols are also essential for Hedgehog signaling, a pathway critical in embryogenesis and cancer. Despite their importance, the use of imaging sterols in cells is currently very limited. We introduce a robust and versatile method for sterol microscopy based on C19 alkyne cholesterol and oxysterol analogues. These sterol analogues are fully functional; they rescue growth of cholesterol auxotrophic cells and faithfully recapitulate the multiple roles that sterols play in Hedgehog signal transduction. Alkyne sterol analogues incorporate efficiently into cellular membranes and can be imaged with high resolution after copper(I)‐catalyzed azide–alkyne cycloaddition reaction with fluorescent azides. We demonstrate the use of alkyne sterol probes for visualizing the subcellular distribution of cholesterol and for two‐color imaging of sterols and choline phospholipids. Our imaging strategy should be broadly applicable to studying the role of sterols in normal physiology and disease.
Physiologia Plantarum | 2014
Hieu Sy Vu; Mary R. Roth; Pamela Tamura; Thilani N. Samarakoon; Sunitha Shiva; Samuel Honey; Kaleb Lowe; Eric A. Schmelz; Todd D. Williams; Ruth Welti
Formation of galactose-acylated monogalactosyldiacylglycerols has been shown to be induced by leaf homogenization, mechanical wounding, avirulent bacterial infection and thawing after snap-freezing. Here, lipidomic analysis using mass spectrometry showed that galactose-acylated monogalactosyldiacylglycerols, formed in wheat (Triticum aestivum) and tomato (Solanum lycopersicum) leaves upon wounding, have acyl-galactose profiles that differ from those of wounded Arabidopsis thaliana, indicating that different plant species accumulate different acyl-galactose components in response to the same stress. Additionally, the composition of the acyl-galactose component of Arabidopsis acMGDG (galactose-acylated monogalactosyldiacylglycerol) depends on the stress treatment. After sub-lethal freezing treatment, acMGDG contained mainly non-oxidized fatty acids esterified to galactose, whereas mostly oxidized fatty acids accumulated on galactose after wounding or bacterial infection. Compositional data are consistent with acMGDG being formed in vivo by transacylation with fatty acids from digalactosyldiacylglycerols. Oxophytodienoic acid, an oxidized fatty acid, was more concentrated on the galactosyl ring of acylated monogalactosyldiacylglycerols than in galactolipids in general. Also, oxidized fatty acid-containing acylated monogalactosyldiacylglycerols increased cumulatively when wounded Arabidopsis leaves were wounded again. These findings suggest that, in Arabidopsis, the pool of galactose-acylated monogalactosyldiacylglycerols may serve to sequester oxidized fatty acids during stress responses.
Beilstein Journal of Nanotechnology | 2016
Dinusha N. Udukala; Hongwang Wang; Sebastian O. Wendel; Aruni P. Malalasekera; Thilani N. Samarakoon; Asanka S. Yapa; Gayani Abayaweera; Matthew T. Basel; Pamela Maynez; Raquel Ortega; Yubisela Toledo; Leonie K. Bossmann; Colette Robinson; Katharine Janik; Olga Koper; Ping Li; Massoud Motamedi; Daniel A. Higgins; Gary L. Gadbury; Gaohong Zhu; Deryl L. Troyer; Stefan H. Bossmann
Summary Proteases, including matrix metalloproteinases (MMPs), tissue serine proteases, and cathepsins (CTS) exhibit numerous functions in tumor biology. Solid tumors are characterized by changes in protease expression levels by tumor and surrounding tissue. Therefore, monitoring protease levels in tissue samples and liquid biopsies is a vital strategy for early cancer detection. Water-dispersable Fe/Fe3O4-core/shell based nanoplatforms for protease detection are capable of detecting protease activity down to sub-femtomolar limits of detection. They feature one dye (tetrakis(carboxyphenyl)porphyrin (TCPP)) that is tethered to the central nanoparticle by means of a protease-cleavable consensus sequence and a second dye (Cy 5.5) that is directly linked. Based on the protease activities of urokinase plasminogen activator (uPA), MMPs 1, 2, 3, 7, 9, and 13, as well as CTS B and L, human breast cancer can be detected at stage I by means of a simple serum test. By monitoring CTS B and L stage 0 detection may be achieved. This initial study, comprised of 46 breast cancer patients and 20 apparently healthy human subjects, demonstrates the feasibility of protease-activity-based liquid biopsies for early cancer diagnosis.
Nanomedicine: Nanotechnology, Biology and Medicine | 2017
Aruni P. Malalasekera; Hongwang Wang; Thilani N. Samarakoon; Dinusha N. Udukala; Asanka S. Yapa; Raquel Ortega; Tej B. Shrestha; Hamad Alshetaiwi; Emily J. McLaurin; Deryl L. Troyer; Stefan H. Bossmann
A nanobiosensor for arginase detection was designed and synthesized. It features a central dopamine-coated iron/iron oxide nanoparticle to which sulfonated cyanine 7.0 is tethered via a stable amide bond. Cyanine 5.5 is linked to the N-terminal of the peptide sequence GRRRRRRRG. Arginine (R) reacts to ornithine (O) in the presence of arginase. Based on calibration with commercially obtained arginase II, the limit of detection (LOD) is picomolar. It is noteworthy that the nanobiosensor for arginase detection does not show a fluorescence increase when incubated with the enzyme NO-reductase, which also uses arginase as substrate, but is indicative of an inflammatory response by the host to cancer and infections. Arginase activity was determined in a syngeneic mouse model for aggressive breast cancer (4T1 tumors in BALB/c mice). It was found that the arginase activity is systemically enhanced, but especially pronounced in the active tumor regions.
Industrial Crops and Products | 2013
Leslie R. Schulte; T. Ballard; Thilani N. Samarakoon; Libin Yao; Praveen V. Vadlani; Scott A. Staggenborg; Mary E. Rezac
Journal of the American Chemical Society | 2013
Ayomi S. Perera; Navaneetha K. Subbaiyan; Mausam Kalita; Sebastian O. Wendel; Thilani N. Samarakoon; Francis D’Souza; Stefan H. Bossmann
Archive | 2010
Stefan H. Bossmann; Deryl L. Troyer; Matthew T. Basel; Thilani N. Samarakoon; Hongwang Wang; Viktor Chikan; Franklin Orban Kroh; Olga Koper; Brandon Walker; Xiaoxuan Leaym