PT  - JOURNAL ARTICLE
AU  - Rogers, Buck E.
AU  - Parry, Jesse J.
AU  - Andrews, Rebecca
AU  - Cordopatis, Paul
AU  - Nock, Berthold A.
AU  - Maina, Theodosia
TI  - MicroPET Imaging of Gene Transfer with a Somatostatin Receptor–Based Reporter Gene and &lt;sup&gt;94m&lt;/sup&gt;Tc-Demotate 1
DP  - 2005 Nov 01
TA  - Journal of Nuclear Medicine
PG  - 1889--1897
VI  - 46
IP  - 11
4099  - http://jnm.snmjournals.org/content/46/11/1889.short
4100  - http://jnm.snmjournals.org/content/46/11/1889.full
SO  - J Nucl Med2005 Nov 01; 46
AB  - Gene therapy trials would benefit greatly from the use of noninvasive imaging to determine the location, magnitude, and time course of gene transfer. Somatostatin receptor subtype 2 (SSTR2) has been used as a reporter probe for γ-camera imaging of gene transfer in animal models. PET has greater sensitivity than γ-camera imaging and therefore would have an advantage for the imaging of SSTR2 gene transfer. Methods: An adenovirus (AdHASSTR2) carrying sstr2, which encodes an N-terminal hemagglutinin epitope, was used for evaluating SSTR2 gene transfer. The somatostatin analog Demotate 1 (Tyr3-octreotate conjugated to the 1,4,8,11-tetraazaundecane chelator) was used for chelation of the positron emitter 94mTc (half-life, 52 min) and targeting to SSTR2. Gene transfer was evaluated in vitro with A-427 non–small cell lung cancer cells after infection with AdHASSTR2 by 94mTc-Demotate 1 binding and internalization assays. In vivo biodistribution and microPET studies were conducted with mice bearing A-427 tumor xenografts directly injected with AdHASSTR2 to determine the tumor localization of 94mTc-Demotate 1. Results: 94mTc-Demotate 1 bound with high affinity and was internalized rapidly into AdHASSTR2-infected A-427 cells. Biodistribution studies showed uptake of 94mTc-Demotate 1 in tumors infected with AdHASSTR2 (4.0 percentage injected dose per gram [%ID/g] at 2 h) and background uptake in tumors infected with a control adenovirus (0.8 %ID/g at 2 h). The uptake of 94mTc-Demotate 1 in AdHASSTR2-infected tumors was greater than the uptake in all other tissues, except for the kidneys and the SSTR2-positive pancreas. MicroPET imaging showed similar results, with clear uptake of 94mTc-Demotate 1 in AdHASSTR2-infected tumors, background uptake in control tumors, and clearance through the kidneys. Conclusion: These studies show that the positron-emitting somatostatin analog 94mTc-Demotate 1 could be used to determine SSTR2 gene transfer by microPET imaging, a result that will improve the sensitivity of the SSTR2 reporter gene system.