Antiangiogenesis Targeting Tumor Microenvironment Synergizes Glucuronide Prodrug Antitumor Activity

Ting-Yi, Juan; Roffler, Steve R.; Hou, Hsien-San; Huang, Shih‐Ming; Chen, Kai-Chuan; Leu, Yu-Ling; Prijovich, Zeljko M.; Yu, Cheng‐Ping; Wu, Chang‐Chieh; Sun, Guang‐Huan; Cha, Tai‐Lung

doi:10.1158/1078-0432.ccr-09-0090

Cited by 50 publications

(48 citation statements)

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“…bG is considered as a tumor marker (14,15,20) and a prodrug-activating enzyme for cancer prodrug therapies (35,36). Connors and Whisson demonstrated that high bG levels present in plasmacytomas were correlated with higher drug sensitivity of the tumors (37).…”

Section: Discussionmentioning

confidence: 99%

“…9-11) and gene-directed enzyme prodrug therapy (GDEPT; refs. 6, 12, 13) as well as directly in prodrug monotherapy, which relies on the elevated levels of bG found in the tumor microenvironment (14)(15)(16) to selectively convert prodrug into active drug. For instance, Albin and colleagues reported that the level of bG human breast tumors was up to 6-times greater than that in normal tissues (17).…”

mentioning

confidence: 99%

“…Elevated levels of bG present in the tumor environment are believed to be due to tumor overexpression (14) and release from necrotic tumor tissues (19) or tumor-infiltrating immune cells (15). Because bG has been considered as a tumor marker (14,15,20), it would be very useful to image bG activity in vivo to personalize glucuronide prodrug treatment and greatly improve exogenous or endogenous bG-based targeted therapy.…”

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confidence: 99%

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PET Imaging of β-Glucuronidase Activity by an Activity-Based 124I-Trapping Probe for the Personalized Glucuronide Prodrug Targeted Therapy

Cheng

Leu

et al. 2014

Molecular Cancer Therapeutics

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Beta-glucuronidase (bG) is a potential biomarker for cancer diagnosis and prodrug therapy. The ability to image bG activity in patients would assist in personalized glucuronide prodrug cancer therapy. However, whole-body imaging of bG activity for medical usage is not yet available. Here, we developed a radioactive bG activity-based trapping probe for positron emission tomography (PET). We generated a 124 I-tyramine-conjugated difluoromethylphenol beta-glucuronide probe (TrapG) to form 124 I-TrapG that could be selectively activated by bG for subsequent attachment of 124 I-tyramine to nucleophilic moieties near bG-expressing sites. We estimated the specificity of a fluorescent FITC-TrapG, the cytotoxicity of tyramine-TrapG, and the serum half-life of 124 I-TrapG. bG targeting of 124 I-TrapG in vivo was examined by micro-PET. The biodistribution of 131 I-TrapG was investigated in different organs. Finally, we imaged the endogenous bG activity and assessed its correlation with therapeutic efficacy of 9-aminocamptothecin glucuronide (9ACG) prodrug in native tumors. FITC-TrapG showed specific trapping at bG-expressing CT26 (CT26/mbG) cells but not in CT26 cells. The native TrapG probe possessed low cytotoxicity. 124 ITrapG preferentially accumulated in CT26/mbG but not CT26 cells. Meanwhile, micro-PET and wholebody autoradiography results demonstrated that 124 I-TrapG signals in CT26/mbG tumors were 141.4-fold greater than in CT26 tumors. Importantly, Colo205 xenografts in nude mice that express elevated endogenous bG can be monitored by using infrared glucuronide trapping probes (NIR-TrapG) and suppressed by 9ACG prodrug treatment. 124 I-TrapG exhibited low cytotoxicity allowing long-term monitoring of bG activity in vivo to aid in the optimization of prodrug targeted therapy.

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Section: Discussionmentioning

confidence: 99%

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confidence: 99%

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confidence: 99%

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PET Imaging of β-Glucuronidase Activity by an Activity-Based 124I-Trapping Probe for the Personalized Glucuronide Prodrug Targeted Therapy

Cheng

Leu

et al. 2014

Molecular Cancer Therapeutics

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“…For instance, Juan and colleagues (29) demonstrated that antiangiogenic agents can synergize the antitumor activity of glucuronide prodrugs by selectively enhancing concentration of the activating enzyme in the tumor microenvironment. More recently, the concept of glucuronidase-responsive albumin-binding prodrugs seemed to represent a promising approach to limiting the rapid renal clearance observed with previous glucuronide prodrugs (46).…”

Section: Discussionmentioning

confidence: 99%

“…In fact, several studies have shown that glucuronide prodrugs can be activated by b-glucuronidase present in high concentrations in necrotic areas of most solid tumors, including glioblastomas (27). b-Glucuronidase is secreted extracellularly in tumors by inflammatory cells such as neutrophils and macrophages, while in healthy tissues, its activity is confined to lysosomes (28,29). This enzymatic specificity of the tumor microenvironment allows glucuronide prodrugs to discriminate between malignant and normal tissues.…”

Section: Introductionmentioning

confidence: 99%

Selective Release of a Cyclopamine Glucuronide Prodrug toward Stem-like Cancer Cell Inhibition in Glioblastoma

Balbous

Renoux

Cortes

et al. 2014

Molecular Cancer Therapeutics

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Recent data suggest that inhibition of the Hedgehog pathway could be a therapeutic target for glioblastoma. Alkaloid cyclopamine inhibits Hedgehog signaling, depleting stem-like cancer cells derived from glioblastoma. However, this compound is toxic for somatic stem cells, preventing its use for clinical applications. In this study, we tested a derivatization product of cyclopamine in the form of cyclopamine glucuronide prodrug (CGP-2). This compound was used in vitro and in vivo toward glioblastoma-initiating cells (GIC). Results obtained in vitro indicate that CGP-2 is active only in the presence of b-glucuronidase, an enzyme detected in high levels in necrotic areas of glioblastomas. CGP-2 decreased proliferation and inhibited the self-renewal of all GIC lines tested. Hedgehog pathway blockade by 10 mmol/L of CGP-2 induced a 99% inhibition of clonogenicity on GICs, similar to cyclopamine treatment. Combination of CGP-2 with radiation decreased clonogenic survival in all GIC lines compared with CGP-2 alone. In a subcutaneous glioblastoma xenograft model, a two-week CGP-2 treatment prevented tumor growth with 75% inhibition at 8 weeks, and this inhibition was still significant after 14 weeks. Unlike cyclopamine, CGP-2 had no detectable toxic effects in intestinal crypts. Our study suggests that inhibition of the Hedgehog pathway with CGP-2 is more effective than conventional temozolomide adjuvant, with much lower concentrations, and seems to be an effective therapeutic strategy for targeting GICs. Mol Cancer Ther; 13(9); 2159-69. Ó2014 AACR.

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A Heterodimeric Glucuronide Prodrug for Cancer Tritherapy: the Double Role of the Chemical Amplifier

et al. 2011

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Antiangiogenesis Targeting Tumor Microenvironment Synergizes Glucuronide Prodrug Antitumor Activity

Cited by 50 publications

References 43 publications

PET Imaging of β-Glucuronidase Activity by an Activity-Based 124I-Trapping Probe for the Personalized Glucuronide Prodrug Targeted Therapy

PET Imaging of β-Glucuronidase Activity by an Activity-Based 124I-Trapping Probe for the Personalized Glucuronide Prodrug Targeted Therapy

Selective Release of a Cyclopamine Glucuronide Prodrug toward Stem-like Cancer Cell Inhibition in Glioblastoma

A Heterodimeric Glucuronide Prodrug for Cancer Tritherapy: the Double Role of the Chemical Amplifier

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