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Dive into the research topics where Susan Ann Cartlidge is active.

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Featured researches published by Susan Ann Cartlidge.


Cancer Research | 2011

Dual IGF-I/II-neutralizing antibody MEDI-573 potently inhibits IGF signaling and tumor growth.

Jin Gao; Jon Chesebrough; Susan Ann Cartlidge; Sally-Ann Ricketts; Leonard Incognito; Margaret Veldman-Jones; David C. Blakey; Mohammad Tabrizi; Bahija Jallal; Pamela A. Trail; Steven Coats; Klaus Bosslet; Yong S. Chang

Insulin-like growth factors (IGF), IGF-I and IGF-II, are small polypeptides involved in regulating cell proliferation, survival, differentiation, and transformation. IGF activities are mediated through binding and activation of IGF-1R or insulin receptor isoform A (IR-A). The role of the IGF-1R pathway in promoting tumor growth and survival is well documented. Overexpression of IGF-II and IR-A is reported in multiple types of cancer and is proposed as a potential mechanism for cancer cells to develop resistance to IGF-1R-targeting therapy. MEDI-573 is a fully human antibody that neutralizes both IGF-I and IGF-II and inhibits IGF signaling through both the IGF-1R and IR-A pathways. Here, we show that MEDI-573 blocks the binding of IGF-I and IGF-II to IGF-1R or IR-A, leading to the inhibition of IGF-induced signaling pathways and cell proliferation. MEDI-573 significantly inhibited the in vivo growth of IGF-I- or IGF-II-driven tumors. Pharmacodynamic analysis demonstrated inhibition of IGF-1R phosphorylation in tumors in mice dosed with MEDI-573, indicating that the antitumor activity is mediated via inhibition of IGF-1R signaling pathways. Finally, MEDI-573 significantly decreased (18)F-fluorodeoxyglucose ((18)F-FDG) uptake in IGF-driven tumor models, highlighting the potential utility of (18)F-FDG-PET as a noninvasive pharmacodynamic readout for evaluating the use of MEDI-573 in the clinic. Taken together, these results demonstrate that the inhibition of IGF-I and IGF-II ligands by MEDI-573 results in potent antitumor activity and offers an effective approach to selectively target both the IGF-1R and IR-A signaling pathways.


Archive | 2006

Binding proteins specific for insulin-like growth factors and uses thereof

Olivia Raeber; Gadi Gazit-Bornstein; Xiaodong Yang; Susan Ann Cartlidge; David William Tonge


Archive | 2007

Targeted binding agents directed to pdgfr-alpha and uses thereof

David Charles Blakey; Susan Ann Cartlidge; Ian Foltz; Gadi Gazit-Bornstein; Jaspal Singh Kang; Naomi Laing; Laura Taylor; Xiao-Dong Yang


Archive | 2008

Binding proteins specific for insulin-like growth factors and uses thereof-909

Vahe Bedian; Susan Ann Cartlidge; Gadi Gazit-Bornstein; Olivia Raeber; David William Tonge; Xiao-Dong Yang


Archive | 2007

Human antibodies to ERBB2

Susan Ann Cartlidge; Jianying Dong; Mark Hickinson; Jaspal Singh Kang; Ian Foltz


Archive | 2007

Human antibodies to erbb 2

Susan Ann Cartlidge; Jianying Dong; Mark Hickinson; Ian Foltz; Jaspal Singh Kang


Archive | 2006

Insulin-like growth factor antibodies and uses thereof

Olivia Raeber; Gadi Gazit-Bornstein; Xiaodong Yang; Susan Ann Cartlidge; David William Tonge


Archive | 2016

Use of an antibody, or antigen-binding fragment thereof, that preferentially binds to insulin-like growth factor-ii (igf-ii) with cross-reactivity to insulin-like growth factor-i (igf-i), in the manufacture of medicaments and as medicaments for the treatment of a malignant tumor in a mammal

David William Tonge; Olivia Raeber; Gadi Gazit-Bornstein; Xiadong Yang; Susan Ann Cartlidge


Archive | 2011

Methods of using insulin-like growth factor antibodies to treat tumors

Olivia Raeber; Gadi Gazit-Bornstein; Xiao-Dong Yang; Susan Ann Cartlidge; David William Tonge


Archive | 2007

Menschliche Antikörper gegen ERBB2

Susan Ann Cartlidge; Jianying Dong; Mark Hickinson; Jaspal Singh Kang; Ian Foltz

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