Inhibition of integrin α<sub>5</sub>β<sub>1</sub> function with a small peptide (ATN‐161) plus continuous 5‐FU infusion reduces colorectal liver metastases and improves survival in mice

Stoeltzing, Oliver; Liu, Wenbiao; Reinmuth, Niels; Fan, Fan; Parry, Graham; Parikh, Alexander A.; McCarty, Marya F.; Bucana, Corazon D.; Mazar, Andrew P.; Ellis, Lee M.

doi:10.1002/ijc.10958

Cited by 206 publications

(161 citation statements)

References 26 publications

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“…Similar to the clinical development of other agents such as bevacizumab (Hurwitz et al, 2004;Wakelee and Schiller, 2005;Ahmed et al, 2004;Rini et al, 2005;Sledge, 2005), the best approach for phase 2 studies will be combinations of ATN-161 with chemotherapy rather than development as a single agent (Plunkett et al, , 2003Stoeltzing et al, 2003).…”

Section: Discussionmentioning

confidence: 99%

“…Attempts to show induction of apoptosis in MLL cells by ATN-161 were unsuccessful, suggesting that the inhibitory effects of ATN-161 on primary tumour growth and metastasis formation were the result of inhibition of new blood vessel growth rather than a direct effect on tumour cells. We have also generated preclinical data showing additive effects with diverse chemotherapy agents Plunkett et al, 2003;Stoeltzing et al, 2003). ATN-161 was not immunogenic in animal studies.…”

mentioning

confidence: 98%

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Phase 1 trial of the antiangiogenic peptide ATN-161 (Ac-PHSCN-NH2), a beta integrin antagonist, in patients with solid tumours

Kimmel²,

et al. 2006

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To evaluate the toxicity, pharmacological and biological properties of ATN-161, a five -amino-acid peptide derived from the synergy region of fibronectin, adult patients with advanced solid tumours were enrolled in eight sequential dose cohorts (0.1 -16 mg kg À1 ), receiving ATN-161 administered as a 10-min infusion thrice weekly. Pharmacokinetic sampling of blood and urine over 7 h was performed on Day 1. Twenty-six patients received from 1 to 14 4-week cycles of treatment. The total number of cycles administered to all patients was 86, without dose-limiting toxicities. At dose levels above 0.5 mg kg À1 , mean total clearance and volume of distribution showed dose-independent pharmacokinetics (PKs). At 8.0 and 16.0 mg kg À1 , clearance of ATN-161 was reduced, suggesting saturable PKs. Dose escalation was halted at 16 mg kg À1 when drug exposure (area under the curve) exceeded that associated with efficacy in animal models. There were no objective responses. Six patients received more than four cycles of treatment (4112 days). Three patients received 10 or more cycles (X280 days). ATN-161 was well tolerated at all dose levels. Approximately, 1/3 of the patients in the study manifested prolonged stable disease. These findings suggest that ATN-161 should be investigated further as an antiangiogenic and antimetastatic cancer agent alone or with chemotherapy.

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Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 98%

Phase 1 trial of the antiangiogenic peptide ATN-161 (Ac-PHSCN-NH2), a beta integrin antagonist, in patients with solid tumours

Kimmel²,

et al. 2006

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“…Once integrins a5b1 and avb3 are expressed, angiogenesis depends on each integrin as antagonists of each can block angiogenesis in vivo (Brooks et al, 1994a, b;Kim et al, 2000a). Antibody and peptide antagonists of integrins avb3 and a5b1 inhibit growth factor as well as tumour angiogenesis, tumour growth and tumour metastasis (Brooks et al, 1994a, b;Carron et al, 1998;Kim et al, 2000a;Stoeltzing et al, 2003). These studies indicate that these integrins function in part by promoting survival in proliferating endothelial cells in vivo (Brooks et al, 1994b;Kim et al, 2002).…”

Section: Integrins Regulate Angiogenesismentioning

confidence: 99%

“…A cyclic peptide inhibitor of integrin avb3/avb5, Cilengitide, is in Phase I/II trials for glioblastoma and other cancers (Burke et al, 2002;Eskens et al, 2003;Smith, 2003). Other promising integrin a5b1-and avb3-blocking peptides with antitumour angiogenesis and tumour metastasis activities are currently in preclinical development (Carron et al, 1998;Reinmuth et al, 2003;Stoeltzing et al, 2003). As Avastin, the antibody inhibitor of VEGF, has recently shown promise as a therapeutic for colon cancer in Phase III clinical trials (Fernando and Hurwitz, 2003), these integrin-based antiangiogenesis therapeutics hold great promise as powerful therapeutics for the treatment of cancer.…”

Section: Integrin Inhibitors As Therapeutic Agents For Cancermentioning

confidence: 99%

Integrins: roles in cancer development and as treatment targets

2004

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The integrin family of cell adhesion proteins promotes the attachment and migration of cells on the surrounding extracellular matrix (ECM). Through signals transduced upon integrin ligation by ECM proteins or immunoglobulin superfamily molecules, this family of proteins plays key roles in regulating tumour growth and metastasis as well as tumour angiogenesis. Several integrins play key roles in promoting tumour angiogenesis and tumour metastasis. Antagonists of several integrins (a5b1, avb3 and avb5) are now under evaluation in clinical trials to determine their potential as therapeutics for cancer and other diseases.

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“…Thus, Hox D3 may provide a switch to activate a program of angiogenesis that includes expression of both during ␣ v ␤ 3 and ␣ 5 ␤ 1 angiogenesis. Once integrins ␣ 5 ␤ 1 and ␣ v ␤ 3 are expressed, angiogenesis depends on each integrin as antagonists of each can block angiogenesis in vivo (10,(15)(16)(17)35).…”

mentioning

confidence: 99%

The Homeobox Transcription Factor Hox D3 Promotes Integrin α5β1 Expression and Function during Angiogenesis

Boudreau

Varner

2004

Journal of Biological Chemistry

129

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Neovascularization promotes wound healing, tumor growth, and arthritis. Endothelial cell migration and survival during neovascularization are regulated by adhesion proteins, including integrin ␣ 5 ␤ 1 . Integrin ␣ 5 ␤ 1 is poorly expressed on normal quiescent blood vessels, but its expression is induced on tumor blood vessels and in response to angiogenic factors such as basic fibroblast growth factor, interleukin-8, tumor necrosis factor-␣, and the angiomatrix protein Del-1. We show here that ␣ 5 ␤ 1 expression, and hence function, during angiogenesis is regulated by the transcription factor Hox D3, a homeobox gene that also controls the expression of endothelial cell integrin ␣ v ␤ 3 and urokinase-type plasminogen activator. Hox D3 expression in endothelial cells enhances integrin ␣ 5 protein and message expression, whereas Hox D3 antisense inhibits its expression. Hox D3 promotes ␣ 5 expression during angiogenesis in vivo, whereas inhibition of ␣ 5 expression by Hox D3 antisense suppresses angiogenesis. Hox D3 binds directly to the promoters of the integrin ␣ 5 and ␤ 3 subunits, inducing subunit expression. As Hox D3, integrin ␣ v ␤ 3 , and integrin ␣ 5 ␤ 1 are expressed on tumor blood vessels but not on normal quiescent vessels, these studies suggest that Hox D3 coordinately regulates the expression of integrin ␣ 5 ␤ 1 and integrin ␣ v ␤ 3 during angiogenesis in vivo. These studies also suggest that Hox D3 inhibition could be a useful approach to inhibit tumor angiogenesis.Angiogenesis, the formation and differentiation of blood vessels from pre-existing vessels or endothelial progenitor cells, is important in both health and disease (1-6). Neovascularization is an important process during embryonic development, wound healing, and reproduction. It also plays an important role in the development of tumors and other diseases such as diabetic retinopathy, age-related macular degeneration, and psoriasis (1-6). Because neovascularization promotes cancer and other diseases, it is important to gain an understanding of the mechanisms by which angiogenesis is regulated.The integrin family of cell adhesion proteins mediates cell attachment to the extracellular matrix and promotes the survival, proliferation, and motility of ECs 1 during angiogenesis (7-18). In fact, at least three integrins receptors for provisional matrix proteins (␣ v ␤ 3 , ␣ v ␤ 5 , and ␣ 5 ␤ 1 ) play important roles in angiogenesis (10, 12, 13, 16 -22). Integrin ␣ 5 ␤ 1 plays a key role in the regulation of angiogenesis, as antagonists of this integrin inhibit angiogenesis (12,16,17). Both ␣ 5 ␤ 1 and its ligand fibronectin are poorly expressed in quiescent endothelium but strongly expressed in proliferating endothelium (16). Expression of integrin ␣ 5 ␤ 1 is up-regulated on human tumor vasculature in breast and colon tumors (16). It is also up-regulated on blood vessels in the brain during wound healing (19). Once expressed, ␣ 5 ␤ 1 regulates the survival and migration of endothelial cells in vitro and in vivo (12,17). Loss of the gene encoding t...

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Inhibition of integrin α₅β₁ function with a small peptide (ATN‐161) plus continuous 5‐FU infusion reduces colorectal liver metastases and improves survival in mice

Cited by 206 publications

References 26 publications

Phase 1 trial of the antiangiogenic peptide ATN-161 (Ac-PHSCN-NH2), a beta integrin antagonist, in patients with solid tumours

Phase 1 trial of the antiangiogenic peptide ATN-161 (Ac-PHSCN-NH2), a beta integrin antagonist, in patients with solid tumours

Integrins: roles in cancer development and as treatment targets

The Homeobox Transcription Factor Hox D3 Promotes Integrin α5β1 Expression and Function during Angiogenesis

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Inhibition of integrin α5β1 function with a small peptide (ATN‐161) plus continuous 5‐FU infusion reduces colorectal liver metastases and improves survival in mice

Cited by 206 publications

References 26 publications

Phase 1 trial of the antiangiogenic peptide ATN-161 (Ac-PHSCN-NH2), a beta integrin antagonist, in patients with solid tumours

Phase 1 trial of the antiangiogenic peptide ATN-161 (Ac-PHSCN-NH2), a beta integrin antagonist, in patients with solid tumours

Integrins: roles in cancer development and as treatment targets

The Homeobox Transcription Factor Hox D3 Promotes Integrin α5β1 Expression and Function during Angiogenesis

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Product

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Inhibition of integrin α₅β₁ function with a small peptide (ATN‐161) plus continuous 5‐FU infusion reduces colorectal liver metastases and improves survival in mice