The Effect of Various Therapeutic Solutions including Colloidal Chromic 32p via an Intratumoral Injection on the Tumor Physiological Parameters of AsPC-1 Human Pancreatic Tumor Xenografts in Nude
نویسندگان
چکیده
To overcome the physiological barrier in solid tumors (i.e., tumor hypertension), a large volume of material is required via an intratumoral injection. Alternatively, a method of reduction in tumor hypertension is also feasible. In this study, we focused on the physiological response after an intratumoral infusion of various therapeutic agents. Tumor interstitial fluid pressure (TIFP) was intermittently monitored for up to 7 days after treatment using AsPC-1 human pancreatic tumors in nude mice. Macroaggregated albumin (MAA), colloidal chromic 32p (32p . cp ) , albumin, dexamethasone, 5-fluoro-2'deoxyuridine, dextrose, saline, and trypan blue increased T I F P within --5 min , a n d T I F P returned to the original level within 1 h, except in the case of MAA and 3 2 p c P . We also found that the maximal uptake for AsPC-1 tumors in both the exponential and plateau growth phases occurred at --100 min postincubation; the m a x i m u m value in the exponential growth phase was 2 times less than that of plateau growth phase (P < 0.01). Therefore, this study supports intralesional 32p-cP brachytherapy for nonresectional pancreatic cancer patients. This may offer a promising treatment modality for delivering high doses of tumor-selective radiation, mainly due to two physiological mechanisms: (a) the high adherence of 32p-cP to the infused regions; and (b) reduction in either tumor blood flow or TIFP by this therapeutic colloid. Presented at the "Seventh Conference on Radioimmunodetection and Radioimmunotherapy of Cancer," October 15-17, 1998, Princeton, NJ. Supported by grants from the New Jersey State Commission on Cancer Research (to I. L.) and the AlfaCell Corp., Bloomfield, New Jersey (to I. L.). This work was performed at the Radiation Research Laboratory, Division of Radiation Research, UMDNJ-Robert Wood Johnson Medical School, Camden, New Jersey. This laboratory was closed in December 1998 due to lack of research funds. 2 To whom requests for reprints should be addressed. Present address: Department of Radiation Oncology, University of Pennsylvania School of Medicine, 195 John Morgan Building, 3620 Hamilton Walk, Philadelphia, PA 19104-6072. Phone: (215) 898-0071 ; Fax: (215) 898-0090, E-mail: ilee2 @ mail.med.upenn.edu, Introduction Rapid advances in the molecular biology of cancer have led to the development of various genetically engineered molecules, including monoclonal antibodies as well as other useful macromolecules. Due to the elevated TIFP, 3 radiolabeled monoclonal antibodies and gene therapy in cancer treatment have not been as effective as anticipated. To overcome this physiological barrier, administration of a large volume of material via an i.t. injection is required. When a therapeutic agent is mixed with a large quantity of fluid directly infused into the center of a tumor, it increases the pressure at the core of the tumor relative to its surroundings. Consequently, the drug spreads along an artificially induced pressure gradient by convection from the core through the surrounding region and into the periphery (1). To elucidate physiological response alter an i.t. infusion (volume, 100 ~xl) of various therapeutic agents, TIFPs were intermittently monitored up to 7 days posttreatment. Several relevant materials such as saline (0.9% or 30% NaC1), 32p-cP, MAA (105 or 10 7 particles), human albumin (--2.5 mg/ml), 30% dextrose, dexamethasone (1 mg/ml), 5-fluoro-2'-deoxyuridine (500 ms/ks) , RNase-like ONC, and trypan blue (0.4%) were used on AsPC-1 human pancreatic carcinoma xenografts in nude mice. This study supports the hypothesis that if 32p-cP was introduced intratumorally, it would maintain highly efficient tumor targeting by 3~P-CP-induced physiological mechanisms. Materials and Methods Animals and Tumors. Female 8-10-week-old nude mice (Cox Animal Facility, Massachusetts General Hospital, Boston, MA) were used, and they were kept under pathogenfree conditions in the vivarium maintained at 25~ + 3~ AsPC-1 tumor cells were cultured, and they were grown in vitro. Single cell suspensions were prepared using 0.25% trypsin solution. About 1 • 106 viable cells suspended in 50 Ixl of HBSS were injected s.c. into the right thighs of mice. Experiments were carried out when the tumor volume was 5 0 0 m m 3 (2). In Vitro 32p-cP Cellular Uptake Measurements. AsPC-1 cells were plated in 24-multiwell plates and then incubated to grow in either the exponential or plateau growth phase. After exposure to 10 p~Ci of 32p-cP (Mallinckrodt Medical, Inc., 3 The abbreviations used are: TIFP, tumor interstitial fluid pressure; i.t., intratumoral; MAA, macroaggregated albumin; 32p-cP, colloidal chromic 32p; TBF, tumor blood flow; ONC, onconase; IFP, interstitial fluid pressure; WIN, wick-in-needle. Research. on April 14, 2017. © 1999 American Association for Cancer clincancerres.aacrjournals.org Downloaded from 3140s Tumor Targeting by an Intratumoral Injection
منابع مشابه
The Effect of Various Therapeutic Solutions including Colloidal Chromic 32p via an Intratumoral Injection on the Tumor Physiological Parameters of AsPC-1 Human Pancreatic Tumor Xenografts in Nude
To overcome the physiological barrier in solid tumors (i.e., tumor hypertension), a large volume of material is required via an intratumoral injection. Alternatively, a method of reduction in tumor hypertension is also feasible. In this study, we focused on the physiological response after an intratumoral infusion of various therapeutic agents. Tumor interstitial fluid pressure (TIFP) was inter...
متن کاملComplete tumor response following intratumoral 32P BioSilicon on human hepatocellular and pancreatic carcinoma xenografts in nude mice.
PURPOSE 32P BioSilicon is a new, implantable, radiological medical device that comprises particles of highly pure silicon encapsulating 32phosphorus (32P) for the treatment of unresectable solid tumors. Prior to administration, the device particles are suspended in a formulant which provides an even suspension of the intended dose for implantation. The primary objective of this animal trial stu...
متن کاملAntitumor effects of 32P-chromic-poly (L-lactide) brachytherapy in nude mice with human prostate cancer
The aim of the present study was to investigate the antitumor effects and tissue distribution of 32P-chromic-poly (L-lactide) (32P-CP-PLLA) in nude mice with human prostate cancer. Tumor models were obtained by transplantation of PC-3M tumor cells into male BALB/c nude mice. Animals were randomly divided into control, 32P-chromic phosphate (32P-CP) colloid and 32P-CP-PLLA groups (all n=20). A s...
متن کامل[Methyl-14C]-choline incorporation into nude mice bearing tumor xenografts-correlation with [methyl-3H]-thymidine: A pilot study
Background: Many in vitro studies suggested that choline incorporation into many types of tumors is related to cell proliferation. Whether in vivo choline incorporation is related also to cell proliferation or not was my question. Therefore, the aim of this pilot study was to investigate the relationship of in vivo [methyl- 14C]-choline incorporation and in vivo [methyl-3H]- thymidine incorpora...
متن کاملDown-regulation of ZIP4 by RNA interference inhibits pancreatic cancer growth and increases the survival of nude mice with pancreatic cancer xenografts.
PURPOSE Zinc levels have been correlated with cancer risk, although the role of zinc and zinc transporters in cancer progression is largely unknown. We recently found that a zinc transporter, ZIP4, is overexpressed in pancreatic cancer. In this study, we further deciphered the role that ZIP4 plays in a pancreatic cancer mouse model by silencing ZIP4. EXPERIMENTAL DESIGN ZIP4 stable silencing ...
متن کامل