Construction of an Immunotoxin, D2C7-(scdsFv)-PE38KDEL, Targeting EGFRwt and EGFRvIII for Brain Tumor Therapy

被引：56

作者：

Chandramohan, Vidyalakshmi ^{[1
,2
]}

Bao, Xuhui ^{[1
,2
,4
]}

Keir, Stephen T. ^{[1
,2
]}

Pegram, Charles N. ^{[1
,2
]}

Szafranski, Scott E. ^{[1
,2
]}

Piao, Hailan ^{[1
,2
]}

Wikstrand, Carol J. ^{[5
]}

McLendon, Roger E. ^{[1
,2
]}

Kuan, Chien-Tsun ^{[1
,2
]}

Pastan, Ira H. ^{[3
]}

Bigner, Darell D. ^{[1
,2
]}

机构：

[1] Duke Univ, Med Ctr, Preston Robert Tisch Brain Tumor Ctr, Durham, NC 27710 USA

[2] Duke Univ, Med Ctr, Dept Pathol, Durham, NC 27710 USA

[3] NCI, NIH, Ctr Canc Res, Mol Biol Lab, Bethesda, MD 20892 USA

[4] Fudan Univ, Huashan Hosp, Dept Neurol, Shanghai 200433, Peoples R China

[5] Saba Univ, Sch Med, Saba, Dutch Caribbean, Netherlands

来源：

CLINICAL CANCER RESEARCH | 2013年 / 19卷 / 17期

关键词：

GROWTH-FACTOR-RECEPTOR; INTEGRATED GENOMIC ANALYSIS; SINGLE-CHAIN IMMUNOTOXIN; PHASE-II TRIAL; MONOCLONAL-ANTIBODY; GLIOBLASTOMA-MULTIFORME; MALIGNANT GLIOMA; EXPRESSION; CELLS; AMPLIFICATION;

D O I：

10.1158/1078-0432.CCR-12-3891

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

Purpose: The EGF receptor gene (EGFR) is most frequently amplified and overexpressed, along with its deletion mutant, EGFRvIII, in glioblastoma. We tested the preclinical efficacy of the recombinant immunotoxin, D2C7-(scdsFv)-PE38KDEL, which is reactive with a 55-amino acid (AA) region present in the extracellular domain of both EGFRwt (583-637 AAs) and EGFRvIII (292-346 AAs) proteins. Experimental Design: The binding affinity and specificity of D2C7-(scdsFv)-PE38KDEL for EGFRwt and EGFRvIII were measured by surface-plasmon resonance and flow cytometry. In vitro cytotoxicity of D2C7-(scdsFv)-PE38KDEL was measured by inhibition of protein synthesis in human EGFRwt-transfected NR6 (NR6W), human EGFRvIII-transfected NR6 (NR6M), EGFRwt-overexpressing A431-epidermoid-carcinoma, and glioblastoma xenograft cells (43, D08-0493MG, D2159MG, and D270MG). In vivo antitumor efficacy of D2C7-(scdsFv)-PE38KDEL was evaluated using 43, NR6M, and D270MG orthotopic tumor models. Results: The KD of D2C7-(scdsFv)-PE38KDEL for EGFRwt and EGFRvIII was 1.6 x 10(-9) mol/L and 1.3 x 10(-9) mol/L, respectively. Flow cytometry with NR6W and NR6M cells confirmed the specificity of D2C7-(scdsFv)-PE38KDEL for EGFRwt and EGFRvIII. The D2C7-(scdsFv)-PE38KDEL IC50 was 0.18 to 2.5 ng/mL on cells expressing EGFRwt (NR6W, A431, 43, and D08-0493MG). The D2C7-(scdsFv)-PE38KDEL IC50 was approximately 0.25 ng/mL on EGFRvIII-expressing cells (NR6M) and on EGFRwt- and EGFRvIII-expressing glioblastoma xenograft cells (D2159MG and D270MG). Significantly, in intracranial tumor models of 43, NR6M, and D270MG, treatment with D2C7-(scdsFv)-PE38KDEL by convection-enhanced delivery prolonged survival by 310% (P = 0.006), 28% (P = 0.002), and 166% (P = 0.001), respectively. Conclusions: In preclinical studies, the D2C7-(scdsFv)-PE38KDEL immunotoxin exhibited significant potential for treating brain tumors expressing EGFRwt, EGFRvIII, or both. (C)2013 AACR.

引用

页码：4717 / 4727

页数：11

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