Targeting a Tumor-Specific Laminin Domain Critical for Human Carcinogenesis

Tran, Misha C.; Rousselle, Patricia; Nokelainen, Pasi; Tallapragada, Supreeti; Nt, Nguyen; Ef, Fincher; Mp, Marinkovich

doi:10.1158/0008-5472.can-07-6160

Cited by 72 publications

(71 citation statements)

References 49 publications

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“…Remarkably, this antibody treatment inhibits SCC tumor proliferation, increases tumor cell apoptosis, and inhibits human SCC tumorigenesis. It does so without impacting normal tissue structure [130].…”

Section: Future Perspectives: Laminin-332 and Cancer Treatmentmentioning

confidence: 99%

Laminin-332-Integrin Interaction: A Target For Cancer Therapy?

Tsuruta

Kobayashi²,

Imanishi³

et al. 2008

CMC

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For many years, extracellular matrix (ECM) was considered to function as a tissue support and filler. However, we now know that ECM proteins control many cellular events through their interaction with cell-surface receptors and cytoplasmic signaling pathways. For example, they regulate cell proliferation, cell division, cell adhesion, cell migration, and apoptosis. We focus in this review on a laminin isoform, laminin-332 (formerly termed laminin-5), a major component of the basement membrane (BM) of skin and other epithelial tissues. It is composed of 3 subunits (α3, β3, and γ2) and interacts with at least two integrin receptors expressed by epithelial cells (α3β1 and α6β4 integrin). Mutations in either laminin-332 or integrin α6β4 result in junctional epidermolysis bullosa, a blistering skin disease, while targeting of laminin-332 by autoantibodies in cicatricial pemphigoid leads to dysadhesion of epithelial cells from their underlying connective tissue. Abnormal expression of laminin-332 and its integrin receptors is also a hallmark of certain tumor types and is believed to promote invasion of colon, breast and skin cancer cells. Moreover, there is emerging evidence that laminin-332 and its protease degradation products are not only found at the leading front of several tumors but also likely induce and/or promote tumor cell migration. Thus, in this review, we focus specifically on the role of laminin-332 and its integrin receptors in adhesion, proliferation, and migration/invasion of cancer cells. Finally, we discuss strategies for the development of laminin-332-based antagonists for the treatment of malignant tumors.

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Section: Future Perspectives: Laminin-332 and Cancer Treatmentmentioning

confidence: 99%

Laminin-332-Integrin Interaction: A Target For Cancer Therapy?

Tsuruta

Kobayashi²,

Imanishi³

et al. 2008

CMC

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“…However, it was later discovered that a specific domain of laminin-332, G45, is present only in tumor tissue and promotes tumor formation and progression. 20 Blocking antibodies against G45 were shown in a pre-clinical model to be effective against SCC tumor formation through blockade of PI3K and ERK signaling, but to have no effect on normal skin homeostasis. 20 This is one of the few examples of targeting specific ECM ligands for cancer therapy, but highlights the need for a deeper understanding of how the role of adhesion signaling and specific ECM ligands differ between various homeostatic and pathologic states.…”

mentioning

confidence: 99%

Focal adhesion complex proteins in epidermis and squamous cell carcinoma

Duperret

Ridky

2013

Cell Cycle

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“…In addition, laminins are central to many human diseases such as, muscular dystrophy type-1A [23], Pierson syndrome, epidermolysis bullosa [24][25][26], laryngo-onychocutaneous syndrome [27], and tumorigenesis [28,29].…”

Section: Composition Of Vertebrate Lamininsmentioning

confidence: 99%

Laminins of Hydra ECM: A Comparative Analysis of Hydra and Vertebrate Laminins Based on Current Genomic and ETS DataBases

Sarras¹

2017

MOJAP

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Targeting a Tumor-Specific Laminin Domain Critical for Human Carcinogenesis

Cited by 72 publications

References 49 publications

Laminin-332-Integrin Interaction: A Target For Cancer Therapy?

Laminin-332-Integrin Interaction: A Target For Cancer Therapy?

Focal adhesion complex proteins in epidermis and squamous cell carcinoma

Laminins of Hydra ECM: A Comparative Analysis of Hydra and Vertebrate Laminins Based on Current Genomic and ETS DataBases

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