R.F. Barth 1, W. Yang 1, R.J. Nakkula 1, W. Tjarks 2, K. Ishita 2, L.C. Wu 3, P.J. Binns 4 and K.J. Riley 5 1 Department of Pathology, 2 Division of Medicinal.

Slides:



Advertisements
Similar presentations
Rolf F. Barth, M.D. Department of Pathology The Ohio State University, Columbus, OH 43210, U.S.A. From Translational BNCT Studies in Animals to Clinical.
Advertisements

H. Koivunoro1, E. Hippelänen1, I. Auterinen2, L. Kankaanranta3, M
Examination of the usefulness as the new boron compound of ACBC-BSH Gen Futamura 1 Shinji Kawabata 1 Shin-Ichi Miyatake 1 Toshihiko Kuroiwa 1 Yoshihide.
Reporter Hung-Jen Hsieh. Non-invasive scintigraphic monitoring of gene expression in a HSV-1 thymidine kinase gene therapy model K.W.MORIN, E.E.KNAUS.
Additive effect of BPA and Gd-DTPA for application in accelerator-based neutron source F. Yoshida, K. Nakai, T. Yamamoto, A. Zaboronok, A. Matsumura Department.
EC917 Eva Gallardo, MD Medical Manager, Biocompatibles UK Drug Eluting Bead: Future Product Applications.
A U87 non-stem U87 stem-like U251 non-stem U251 stem-like MFI/FOV:TLR9 ** ,000 1,400 MFI/FOV:pSTAT ,200 ***
T argeting S phingosine K inase 1 and A poptosis by M etformin to D ecrease T umor R esistance to A driamycin By Dr. Ahmed Mohamed Kabel Pharmacology.
第三章 Survivin siRNA nano particles are capable of inhibiting liver cancer cell growth both in vitro and in vivo Suoqin Tang,MD, Kuiyao Qu,MD, Yi Zhang,MD.
Lenalidomide plus dexamethasone is more effective than dexamethasone alone inpatients with relapsed or refractory multiple myeloma regardless of prior.
Lund University, LUND Sweden
Biodistribution of 212Pb Conjugated Trastuzumab in Mice
Camacho et al, Fig. S1 a c e b d f
PARPi-FL - a Fluorescent PARP1 Inhibitor for Glioblastoma Imaging
Introduction Conclusions
Saikosaponin-D Enhances Radiosensitivity of Hepatoma Cells under Hypoxic Conditions by Inhibiting Hypoxia-Inducible Factor-1α Cell Physiol Biochem 2014;33:37-51.
Volume 14, Issue 3, Pages (September 2006)
Fig. 1. Electroporation of interleukin 12 (IL-12) DNA compared with control DNA increases the level of IL-12 expression (picograms/milligrams total protein)
R E I G T T RADIO ELECTRO IMMUNO-GENE TUMOUR THERAPY
Volume 10, Issue 2, Pages (August 2004)
Cyclin-Dependent Kinase 2 Promotes Tumor Proliferation and Induces Radio Resistance in Glioblastoma  Jia Wang, Tong Yang, Gaofeng Xu, Hao Liu, Chunying.
Immunotherapy with Dendritic Cells Modified with Tumor-Associated Antigen Gene Demonstrates Enhanced Antitumor Effect Against Lung Cancer  Tao Jiang,
Yunguang Sun, PhD, Luigi Moretti, MD, Nicholas J
Volume 41, Issue 4, Pages (October 2004)
In vivo gene transfer of pigment epithelium-derived factor inhibits tumor growth in syngeneic murine models of thoracic malignancies  Ali Mahtabifard,
Volume 15, Issue 2, Pages (February 2007)
by Norman Nausch, Ioanna E
Volume 21, Issue 2, Pages (February 2013)
The Zinc Ionophore PCI-5002 Radiosensitizes Non-small Cell Lung Cancer Cells by Enhancing Autophagic Cell Death  Kwang Woon Kim, PhD, Christina K. Speirs,
Brian Hutzen, Chun-Yu Chen, Pin-Yi Wang, Les Sprague, Hayley M
by Bindu Varghese, Adam Widman, James Do, Behnaz Taidi, Debra K
Volume 24, Issue 8, Pages (August 2016)
Vaccination regimens incorporating CpG-containing oligodeoxynucleotides and IL-2 generate antigen-specific antitumor immunity from T-cell populations undergoing.
Measles Virus Entry Through the Signaling Lymphocyte Activation Molecule Governs Efficacy of Mantle Cell Lymphoma Radiovirotherapy  Tanner S Miest, Marie.
Recombinant mumps virus as a cancer therapeutic agent
AMP Is a True Physiological Regulator of AMP-Activated Protein Kinase by Both Allosteric Activation and Enhancing Net Phosphorylation  Graeme J. Gowans,
Telephone    Provider of Global Contract Research Services Accelerating Preclinical Research, Drug Discovery.
Fig. 4. Antitumor efficacy of ERY974 against various cancer types.
Inhibition of FGFR signaling and tumor growth in SNU-16 xenograft model by administration of E7090. Inhibition of FGFR signaling and tumor growth in SNU-16.
Volume 3, Issue 1, Pages (January 2003)
Genetically Engineered Multilineage-Differentiating Stress-Enduring Cells as Cellular Vehicles against Malignant Gliomas  Tomohiro Yamasaki, Shohei Wakao,
Volume 18, Issue 11, Pages (November 2010)
Volume 7, Issue 2, Pages (February 2003)
Volume 18, Issue 3, Pages (March 2010)
Volume 15, Issue 5, Pages (May 2007)
Volume 19, Issue 10, Pages (October 2011)
Volume 22, Issue 1, Pages (January 2014)
Incorporation of the B18R Gene of Vaccinia Virus Into an Oncolytic Herpes Simplex Virus Improves Antitumor Activity  Xinping Fu, Armando Rivera, Lihua.
Select Cancer Testes Antigens of the MAGE-A, -B, and -C Families Are Expressed in Mast Cell Lines and Promote Cell Viability In Vitro and In Vivo  Bing.
Interleukin-18 and the Costimulatory Molecule B7-1 Have a Synergistic Anti-Tumor Effect on Murine Melanoma; Implication of Combined Immunotherapy for.
Molecular Therapy - Nucleic Acids
Reovirus FAST Protein Enhances Vesicular Stomatitis Virus Oncolytic Virotherapy in Primary and Metastatic Tumor Models  Fabrice Le Boeuf, Simon Gebremeskel,
Volume 25, Issue 7, Pages (July 2017)
Volume 17, Issue 2, Pages (February 2009)
Telephone    Provider of Global Contract Research Services Accelerating Preclinical Research, Drug Discovery.
Volume 19, Issue 6, Pages (June 2011)
Molecular Therapy - Oncolytics
Volume 26, Issue 1, Pages (January 2018)
Volume 23, Issue 1, Pages (January 2015)
Volume 22, Issue 3, Pages (March 2014)
Molecular Therapy - Oncolytics
Volume 11, Issue 3, Pages (March 2005)
Cowpox Virus: A New and Armed Oncolytic Poxvirus
Volume 24, Issue 10, Pages (October 2016)
GR cells are dependent upon sustained CDC25C signaling as pharmacologic or genetic inhibition of CDC25C induce synthetic lethality. GR cells are dependent.
The Enhanced Tumor Specificity of TG6002, an Armed Oncolytic Vaccinia Virus Deleted in Two Genes Involved in Nucleotide Metabolism  Johann Foloppe, Juliette.
Gemcitabine-Incorporated G-Quadruplex Aptamer for Targeted Drug Delivery into Pancreas Cancer  Jun Young Park, Ye Lim Cho, Ju Ri Chae, Sung Hwan Moon,
Volume 20, Issue 6, Pages (June 2012)
Volume 18, Issue 2, Pages (February 2010)
In vivo tumor targeting and biodistribution of radiolabeled anti-CEA Fab-H-2Kb/ova conjugates. In vivo tumor targeting and biodistribution of radiolabeled.
Presentation transcript:

R.F. Barth 1, W. Yang 1, R.J. Nakkula 1, W. Tjarks 2, K. Ishita 2, L.C. Wu 3, P.J. Binns 4 and K.J. Riley 5 1 Department of Pathology, 2 Division of Medicinal Chemistry, 3 Department of Molecular Virology, Immunology and Medical Genetics, The Ohio State University, Columbus, OH Department of Radiology, Mt. Auburn Hospital, Cambridge, MA Department of Radiation Oncology, Massachusetts General Hospital, Boston, MA Evaluation of Carboranyl Thymidine Analogues as Potential Delivery Agents for Boron Neutron Capture Therapy

Introduction We have had a longstanding interest in carboranyl nucleosides as potential boron delivery agents for Neutron Capture Therapy (NCT). Among these are carboranyl thymidine analogues (CTAs), which are substrates for thymidine kinase-1 (TK1) and is only expressed in proliferating cells, including a wide variety of a malignant tumors. As has been previously reported by us, a panel of 3-carboranyl Thd analogues (3CTAs) have been designed and synthesized. One of these, designated N5-2OH, previously has been evaluated in vivo using two tumor model systems, the murine L929 tumor in nude mice to validate target specificity and the RG2 rat glioma in Fischer rats to evaluate its therapeutic efficacy. In the present report we describe additional studies with N5-2OH using the F98 and RG2 rat glioma model and data on two recently synthesized CTAs designated 18a and 18b.

Chemical Structures and Formulas of Carboranyl Thymidine Analogues

Western Blot Analysis of Thymidine Kinase 1 Expression in Glioma and L929 Cell Lines MW marker (kDa) hTK1 (ng) F98 RG2 L929TK- L929TK+ TK1 beta-actin F98 RG2 L929TK- L929TK+

Target Validation of L929 TK1(+) and (-) Tumors Following i.t. Injection of N5-2OH and BNCT TK1(+) (  ); TK1(-) (  ); TK1(+) radiation control (  ); TK1(+) untreated control (  ). The vertical lines indicate the standard deviations (SD) of the mean tumor volumes. Animals bearing TK1(+) tumors, which had received N5-2OH by i.t. injection followed by BNCT, had a 15 fold inhibition in growth with a tumor volume of 247±151 mm 3 compared to 3603±1103 mm 3 for matched control animals that did not receive BNCT and 2225±1074 mm 3 for radiated controls that did not receive N5-2OH. Animals bearing L929 TK1(-) tumors showed modest reductions in tumor volumes (Proc. Natl. Acad. Sci. 105: , 2008).

F98 Rat Glioma Model

Biodistribution and Physical Radiation Doses Following Administration of N5-2OH Boron uptake (ID%/g) ‡ Physical dose (Gy) ¶ Group † TumorBrain * Blood Tumor/ Brain Conc. Ratio TumorBrain F98/CED N5-2OH17.3±4.3< F98/CED N5-2OH + i.v. BPA 28.0±4.54.0±1.35.5± F98/i.v. BPA10.7± ±1.15.2± F98/ Irradiation control (CED of DMSO) None B enriched N5-2OH was administered i.c. by means of convection enhanced delivery over 24 h using ALZET ® pumps at a flow rate of 8.33 μL/h. BPA was administered intravenously 2.5 h prior to BNCT. † F98 glioma cells were implanted into rats intracerebrally. The rats were irradiated 14 days after implantation. ‡ Boron content was quantified by means of DCP-AES. Boron uptake was present percent injected dose per gram tissue ( ID%/g) * Boron concentrations for the tumor bearing cerebral hemisphere after excision of the tumor. ¶ Physical dose estimates include contributions from γ photons, 14 N (n,p) 14 C and 10 B (n,  ) 7 Li reactions

Survival Times of F98 Glioma-Bearing Rats Following CED of N5-2OH With or Without i.v. BPA Group † No Survival time (days) * % Increased life span Mean±SE Median RangeMeanMedian CED of N5-2OH + i.v. BPA 843.5± CED of N5-2OH 937.9± i.v. BPA ± Irradiated Controls 831.3± Untreated Controls 725.4± * Mean and median survival times were determined for each group of 7-10 rats. ¶ Percent increased life span (%ILS) was defined relative to mean and median survival times of untreated controls. † N5-2OH and BPA were administered as described in footnotes in Tables 1 and 2.

Survival Plots of F98 Glioma Bearing Rats Survival times have been plotted for untreated animals (●), irradiated controls (○), and animals that received i.v. BPA (♦) or N5-2OH either alone (▲) or in combination with BPA (  ).

Survival Plots of RG2 Glioma Bearing Rats Kaplan-Meier survival plots for RG2 glioma bearing rats. Survival times have been plotted for for untreated animals (●), irradiated controls (○), and animals that received i.v. BPA (♦) or N5-2OH either alone (▲) or in combination with BPA (  ).

Chemical Structures and Formulas of Carboranyl Thymidine Analogues

Biodistribution of Carboranyl Thymidine Analogues N5-20H, 18a and 18b in RG2 Glioma Bearing Rats a Boron concentrations (µg/g) Ratios Test agent b % Boron c and µg Boron TumorR. BrainL. BrainBlood T/BrT/Bl N5-2OH ± ± ± ± a ± ± ± ± b ± ± ± ± a RG2 gliomas (105 cells/10µl) were implanted stereotactically into the right caudate nucleus of syngeneic Fischer rats Biodistribution studies were initiated 14 d. later. b The test agents in a volume of 200 µl were administered i.c. by means of ALZET pumps (model #2001D) over 24hrs at a flow rate of 8.33µl/h. Rats were euthanized immediately thereafter, and their brains and blood were taken for boron determinations by ICP-OES. c % boron was based on the respective molecular weights of N5-2OH (528.65), 18a (427.51) and 18b (417.7).

Mass Spect Studies (neg mode) to Determine in vivo Phosphorylation of the RG2 Glioma [18a-MP + K] - Int.: 436

Conclusions Relating to CTAs as Boron Delivery Agents 1.Strong TK1 expression was demonstrated by Western blot analysis of the F98 and RG2 glioma and the L929 TK1 (+) cell lines. 2.Target validation previously was established using the L929 TK1 (+) and mutant TK1 (-) cell lines (PNAS 105:17493, 2008). 3. In vivo BNCT studies with the F98 glioma model have demonstrated that intracerebral CED of N5-2OH yielded survival data that were equivalent to those obtained with i.v. administration of BPA. 4.The combination of N5-2OH and BPA resulted in a modest increase in MST of F98 glioma bearing rats compared to a statistically significant increase (P= ) in RG2 glioma bearing rats 52.9 vs. 43.5d (PNAS 105, 2008).

5. In vivo biodistribution studies of 18a following i.c. administration by Alzet pumps to RG2 glioma bearing rats showed enhanced uptake compared to N5-2OH. 6. Metabolic mass spectrometric studies indicated the possible formation of monophosphates of N5-2OH and 18a in RG2 glioma cells in vivo. 7. Enzyme kinetic studies have shown that 18a is a 2-3x better substrate of hTK1 than N5-2OH (J. Med. Chem. 48:1188, 2005). 8. Further in vivo studies are warranted to determine if 18a is superior to N5-2OH as a boron delivery agent for NCT.