Department of Medicine, Section of Medical Oncology, Baylor College of Medicine, Houston, Texas 77030, USA.
Clin Cancer Res. 2011 Nov 15;17(22):7174-82. doi: 10.1158/1078-0432.CCR-11-1899. Epub 2011 Sep 20.
GLIPR1 is upregulated by p53 in prostate cancer cells and has preclinical antitumor activity. A phase I clinical trial was conducted to evaluate the safety and activity of the neoadjuvant intraprostatic injection of GLIPR1 expressing adenovirus for intermediate or high-risk localized prostate cancer before radical prostatectomy (RP).
Eligible men had localized prostate cancer (T1-T2c) with Gleason score greater than or equal to 7 or prostate-specific antigen 10 ng/mL or more and were candidates for RP. Patients received the adenoviral vector expressing the GLIPR1 gene by a single injection into the prostate followed four weeks later by RP. Six viral particle (vp) dose levels were evaluated: 10(10), 5 × 10(10), 10(11), 5 × 10(11), 10(12), and 5 × 10(12) vp.
Nineteen patients with a median age of 64 years were recruited. Nine men had T1c, 4 had T2a, and 3 had T2b and T2c clinical stage. Toxicities included urinary tract infection (n = 3), flu-like syndrome (n = 3), fever (n = 1), dysuria (n = 1), and photophobia (n = 1). Laboratory toxicities were grade 1 elevated AST/ALT (n = 1) and elevations of PTT (n = 3, with 1 proven to be lupus anticoagulant). No pathologic complete remission was seen. Morphologic cytotoxic activity, induction of apoptosis, and nuclear p27(Kip1) upregulation were observed. Peripheral blood CD8(+), CD4(+), and CD3(+) T-lymphocytes were increased, with upregulation of their HLA-DR expression and elevations of serum IL-12.
The intraprostatic administration of GLIPR1 tumor suppressor gene expressed by an adenoviral vector was safe in men, with localized intermediate or high-risk prostate cancer preceding RP. Preliminary evidence of biologic antitumor activity and systemic immune response was documented.
GLIPR1 在前列腺癌细胞中受 p53 上调,具有临床前抗肿瘤活性。进行了一项 I 期临床试验,以评估在根治性前列腺切除术 (RP) 前,对局部中高危前列腺癌患者进行 GLIPR1 表达腺病毒的经尿道前列腺内注射的安全性和活性。
符合条件的男性患有局部前列腺癌 (T1-T2c),Gleason 评分≥7 或前列腺特异性抗原≥10ng/mL,且适合 RP。患者接受单次注射 GLIPR1 基因表达的腺病毒载体,四周后进行 RP。评估了 6 种病毒粒子 (vp) 剂量水平:10(10)、5×10(10)、10(11)、5×10(11)、10(12)和 5×10(12)vp。
19 名中位年龄 64 岁的患者入选。9 名男性为 T1c,4 名男性为 T2a,3 名男性为 T2b 和 T2c 临床分期。毒性包括尿路感染 (n=3)、流感样综合征 (n=3)、发热 (n=1)、尿痛 (n=1)和畏光 (n=1)。实验室毒性为 1 级 AST/ALT 升高 (n=1)和 PTT 升高 (n=3,其中 1 例证实为狼疮抗凝物)。未见病理完全缓解。观察到形态学细胞毒性活性、细胞凋亡诱导和核 p27(Kip1)上调。外周血 CD8(+)、CD4(+)和 CD3(+)T 淋巴细胞增加,其 HLA-DR 表达上调,血清 IL-12 升高。
在 RP 前,局部中高危前列腺癌患者经尿道前列腺内给予 GLIPR1 肿瘤抑制基因表达的腺病毒载体是安全的。初步证明了生物抗肿瘤活性和全身免疫反应的证据。
