Morphoproteomic and Molecular Concomitants of an Overexpressed and Activated mTOR Pathway in Renal Cell Carcinomas

Morphoproteomic and Molecular Concomitants of an Overexpressed and Activated mTOR Pathway in Renal Cell Carcinomas

Fan Lin¹, Ping L. Zhang¹, Ximing J. Yang³, Jeffrey W. Prichard¹, Mingyue Lun² and Robert E. Brown¹
¹ Division of Laboratory Medicine and ² Weis Center for Research, Geisinger Medical Center, Danville, Pennsylania; ³ Northwestern Memorial Hospital, Chicago, Illinois

Address correspondence to Robert E. Brown, M.D., at his present address: Department of Pathology, University of Texas Houston Medical School, 6431 Fannin Street, Room 2.286, Houston, TX 77030, USA; tel 713 500 5442; fax 713 500 0732; e-mail robert.brown{at}uth.tmc.edu.

CCI-779 (temsirolimus), an ester of rapamycin and an inhibitorof the mammalian target of rapamycin (mTOR), is currently inphase II trials for treatment of patients with solid cancers.The mTOR functions as a checkpoint for cell proliferation, withupstream Akt and downstream p70S6K serving as its most importantmediators. The aim of this study was to evaluate the expressionand activation of the Akt-mTOR-p70S6K pathway in renal cellcarcinoma (RCC), seeking to strengthen the rationale for targetedtherapy of RCC using rapamycin or a rapamycin analogue. Tissuemicroarray sections containing 128 primary RCCs, 22 metastaticRCCs, and 24 non-neoplastic (normal) kidneys (NK) were immunostainedwith monoclonal antibodies to phosphorylated (p)-Akt (Ser473),p-mTOR (Ser2448), and p-p70S6K (Thr389). Western blotting wasperformed on 3 cases of clear cell RCC (CRCC) and the correspondingnon-neoplastic (normal) renal tissues using the same antibodies.The immunostain scoring system included: (a) location; (b) distribution;and (c) intensity. The normal kidneys provided baseline scoresfor comparison. Expression of p-Akt, p-mTOR, and p-p70S6K wasseen in 100% (n = 24) of NKs and nearly 100% (n = 150) of bothprimary and metastatic RCCs. The p-p70S6K was located in thenucleus in both NKs and RCCs. The p-Akt was observed in thenucleus and cytoplasm of NKs and in the nucleus and cytoplasm/membrane (plasmalemma) of RCCs. The p-mTOR was identified inthe membrane of NKs and the membrane/nucleus of RCCs. The levelsof expression of p-p70S6K, p-mTOR, and p-Akt were significantlyhigher in RCC than in NK in the overall pattern (intensity anddistribution, p <0.05). Western blotting also showed higherexpression of p-p70S6K, p-mTOR, and p-Akt in RCCs compared tothe corresponding normal kidney tissues (p <0.05). Thesefindings indicate that correlative over-expression and activationof p-Akt, p-mTOR, and p-p70S6K are commonly observed in RCCs.After considering these findings in the context of other establishedprotein circuitries and pathways in RCC, we propose therapeuticapproaches that incorporate rapamycin-like agents and othersmall molecule inhibitors in a combinatorial fashion in futureclinical trials for RCC.

Keywords: rapamycin, p-Akt, p-mTOR, p-p70S6K, renal cell carcinoma

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