PT  - JOURNAL ARTICLE
AU  - Jun Liu
AU  - Asghar Hajibeigi
AU  - Gang Ren
AU  - Mai Lin
AU  - Wasana Siyambalapitiyage
AU  - Zhisu Liu
AU  - Evan Simpson
AU  - Robert W. Parkey
AU  - Xiankai Sun
AU  - Orhan K. Öz
TI  - Retention of the Radiotracers &lt;sup&gt;64&lt;/sup&gt;Cu-ATSM and &lt;sup&gt;64&lt;/sup&gt;Cu-PTSM in Human and Murine Tumors Is Influenced by MDR1 Protein Expression
AID  - 10.2967/jnumed.109.061879
DP  - 2009 Aug 01
TA  - Journal of Nuclear Medicine
PG  - 1332--1339
VI  - 50
IP  - 8
4099  - http://jnm.snmjournals.org/content/50/8/1332.short
4100  - http://jnm.snmjournals.org/content/50/8/1332.full
SO  - J Nucl Med2009 Aug 01; 50
AB  - Tumor hypoxia is often associated with resistance to chemotherapy. Multidrug resistance type 1 (MDR1) protein is a member of the adenosine triphosphate binding cassette (ABC) proteins, some of which are involved in the multidrug resistance (MDR) phenotype in tumors. Many studies have focused on the role of these proteins in modulating drug resistance, but their effect on retention of imaging agents is less well studied. To study the role of MDR1 expression on the accumulation of 64Cu-diacetyl-bis(N4-methylthiosemicarbazone) (64Cu-ATSM) and 64Cu-pyruvaldehyde-bis(N4-methylthiosemicarbazone) (64Cu-PTSM) in human tumors in vitro and in vivo, we used a model system composed of a low MDR1–expressing parent uterine sarcoma cell line and a daughter cell line selected for overexpression of MDR1. Aromatase knockout (ArKO) mice that spontaneously developed liver tumors were used as an additional in vivo model to study the effect of MDR expression on 64Cu-ATSM and -PTSM retention. Methods: Biodistribution experiments after injection of 64Cu-ATSM or -PTSM were performed in wild-type mice, ArKO mice, and ArKO mice bearing liver tumors (n = 3–5/group), and in nude mice bearing human tumor xenografts for in vivo PET/CT. Liver expression of Abcb1a and Abcb1b, the MDR1 proteins in mouse liver, was determined by real-time polymerase chain reaction. 64Cu-ATSM and -PTSM accumulation and efflux studies were conducted in tumor cell lines. The uptake experiments were repeated after knockdown of MDR1 protein expression using MDR1-specific small interfering RNAs. Results: In vivo, the hepatic tumors had a lower percentage injected dose per gram of 64Cu-ATSM or -PTSM and more highly expressed Abcb1b than did wild-type liver or nontumor-bearing ArKO liver. High MDR1–expressing tumors showed lower tracer activity on PET/CT images. In vitro, cells highly expressing MDR1 had significantly decreased 64Cu-ATSM and -PTSM retention and enhanced efflux. Knockdown of MDR1 expression significantly enhanced the 64Cu-ATSM and -PTSM retention and decreased the efflux in MDR1-positive cells. Conclusion: The expression of MDR1 glycoprotein (or its equivalents in mice) affects the retention of 64Cu-ATSM and -PTSM in the human and murine tumors tested. These results may have implications for clinical hypoxia imaging in tumors and the therapeutic efficacy of 64Cu-ATSM.