Loss of Survivin in the Prostate Epithelium Impedes Carcinogenesis in a Mouse Model of Prostate Adenocarcinoma

Helty Adisetiyo,Mengmeng Liang,Pradip Roy-Burman,Shili Xu,Chun-Peng Liao,Edward M Conway,Michael B Cohen,Nouri Neamati,Chieh-Yang Cheng,Alexander Yu Nikitin,Ari Aycock-Williams,Hari Koul

doi:10.1371/journal.pone.0069484

Abstract

The inhibitor of apoptosis protein survivin is expressed in most cancers. Using the conditional PTEN deletion mouse model, we previously reported that survivin levels increase with prostate tumor growth. Here we evaluated the functional role of survivin in prostate tumor growth. First, we demonstrated that mice lacking the survivin gene in prostate epithelium were fertile and had normal prostate growth and development. We then serially, from about 10–56 weeks of age, evaluated histopathologic changes in the prostate of mice with PTEN deletion combined with survivin mono- or bi-allelic gene deletion. While within this time period most of the animals with wild-type or monoallelic survivin deletion developed adenocarcinomas, the most severe lesions in the biallelic survivin deleted mice were high-grade prostatic intra-epithelial neoplasia with distinct histopathology. Many atypical cells contained large hypertrophic cytoplasm and desmoplastic reaction in the prostatic intra-epithelial neoplasia lesions of this group was minimal until the late ages. A reduced proliferation index as well as apoptotic and senescent cells were detected in the lesions of mice with compound PTEN/survivin deficiency throughout the time points examined. Survivin deletion was also associated with reduced tumor expression of another inhibitor of apoptosis member, the X-linked inhibitor of apoptosis. Our findings suggest that survivin participates in the progression of prostatic intraepithelial neoplasia to adenocarcinoma, and that survivin interference at the prostatic intraepithelial neoplasia stages may be a potential therapeutic strategy to halt or delay further progression.

Highlights

Survivin is a 142-amino acid residue protein that belongs to the family of inhibitor of apoptosis proteins (IAP)
We proceeded to delete one or both alleles of Survivin in the Pten deletion model, and through analyses of these new strains we provide direct genetic evidence that loss of survivin expression in the prostate epithelium strongly inhibits the progression of prostatic premalignant lesions to adenocarcinoma in these animals
Survivin stands as a unique member of the IAP family with essential roles in mitosis, cellular stress response and inhibition of cell death

Summary

Introduction

Survivin is a 142-amino acid residue protein that belongs to the family of inhibitor of apoptosis proteins (IAP). Due to its high expression in most human cancers and its role in promoting cell proliferation and inhibiting apoptosis, it is considered to be a potentially important therapeutic target [1]. It is thought that survivin over-expression might allow accumulation of mutations in transformed cells and thereby promoting tumor progression. Its expression is associated with increased resistance to cancer therapy-induced apoptosis and with lower patient survival [2]. Survivin contains a single baculoviral inhibitor of apoptosis repeat (BIR) domain and carboxyl terminal α-helix and takes form as a homodimer. Rather than binding directly to caspases, survivin blocks apoptosis by interacting with other partners including XIAP [3,4]

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