Paclitaxel Derivatives for Targeted Therapy of Cancer:  Toward the Development of Smart Taxanes

Safavy, Ahmad; Raisch, Kevin P.; Khazaeli, M. B.; Buchsbaum, Donald J.; Bonner, James A.

doi:10.1021/jm990355x

Cited by 100 publications

(111 citation statements)

References 29 publications

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“…As no reported PKM2 activators exhibit cellular activity, the antitumor drug Taxol was selected as positive control to test the sensitivity of the model. As shown in Table 2, the result of Taxol was consistent with previous reports, 30,31 confirming the accuracy of our experiment. The IC 50 values of tested compounds against different tumor cells ranged between 0.64 and 5.6 µM.…”

Section: Growth Inhibitory Activity On Cancer Cell Linessupporting

confidence: 92%

New pyridin-3-ylmethyl carbamodithioic esters activate pyruvate kinase M2 and potential anticancer lead compounds

Zhang

Liu

et al. 2015

Bioorganic & Medicinal Chemistry

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Section: Growth Inhibitory Activity On Cancer Cell Linessupporting

confidence: 92%

New pyridin-3-ylmethyl carbamodithioic esters activate pyruvate kinase M2 and potential anticancer lead compounds

Zhang

Liu

et al. 2015

Bioorganic & Medicinal Chemistry

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“…AN-215 has been shown more effective than its nontargeted cytotoxic radical, AN-201 in preclinical models of various malignancies, such as SCLC, gastric carcinoma, prostate cancer, and glioblastoma (41 -44). Recently, the synthesis of paclitaxel derivatives of bombesin analogues has been reported (45).…”

Section: Discussionmentioning

confidence: 99%

Effective Inhibition of Experimental Human Ovarian Cancers with a Targeted Cytotoxic Bombesin Analogue AN-215

Engel

Keller

Schally

et al. 2005

Clinical Cancer Research

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Purpose: To determine whether the cytotoxic analogue of bombesin/gastrin-releasing peptide (GRP) AN-215 can inhibit the in vivo growth of four human ovarian cancer cell lines. AN-215 consists of 2-pyrrolinodoxorubicin (AN-201), a superactive derivative of doxorubicin linked to a bombesin antagonist carrier des-D-Tpi-RC-3095. This conjugate binds strongly to receptors for bombesin/GRP and can be targeted to tumors that express these receptors. Bombesin/GRP receptors are found in 77% of human ovarian cancer specimens.Experimental Design: Nude mice bearing xenografts of ES-2, SKOV-3, OV-1063, and UCI-107 human ovarian carcinomas were treated with AN-215. The antitumor effects and the toxicity were determined. The expression of bombesin receptor subtypes was measured by reversetranscriptase PCR analysis, and the presence of bombesin/ GRP receptors was determined by radioligand binding assays.Results: AN-215 significantly (P < < 0.05) inhibited growth of ES-2, OV-1063, and UCI-107 tumors, prevented the metastatic spread of ES-2 cancers, and prolonged the survival of nude mice bearing i.p. ES-2 xenografts. Cytotoxic radical AN-201, the unconjugated mixture of bombesin antagonist RC-3095 and AN-201 or RC-3095 alone had no significant effects. Blockade of bombesin/GRP receptors abolished the effect of AN-215. The expression of bombesin/GRP receptors was not changed after repeated treatment with AN-215.Conclusions: Our findings indicate that targeted chemotherapy with cytotoxic bombesin/GRP analogue AN-215 can inhibit ovarian tumors, which express bombesin/GRP receptors. AN-215 might provide a new treatment modality for women with advanced ovarian carcinoma.

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“…59 The cytotoxicity against H1299 human non small cell lung cancer was enhanced compared with unconjugated taxol. Recently, a multiligand compound, consisting of two BN [6][7][8][9][10][11][12][13][14] and one paclitaxel with enhanced cytotoxic activity against several GRP-R positive human cancer cell lines was synthesized.…”

Section: Drug Linked or Radiolabeled Bn/grp Analogsmentioning

confidence: 98%

Targeting gastrin releasing peptide receptors: New options for the therapy and diagnosis of cancer

Hohla

Schally²

2010

Cell Cycle

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Paclitaxel Derivatives for Targeted Therapy of Cancer: Toward the Development of Smart Taxanes

Cited by 100 publications

References 29 publications

New pyridin-3-ylmethyl carbamodithioic esters activate pyruvate kinase M2 and potential anticancer lead compounds

New pyridin-3-ylmethyl carbamodithioic esters activate pyruvate kinase M2 and potential anticancer lead compounds

Effective Inhibition of Experimental Human Ovarian Cancers with a Targeted Cytotoxic Bombesin Analogue AN-215

Targeting gastrin releasing peptide receptors: New options for the therapy and diagnosis of cancer

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