Pro-nerve Growth Factor Induces Autocrine Stimulation of Breast Cancer Cell Invasion through Tropomyosin-related Kinase A (TrkA) and Sortilin Protein

Demont, Yohann; Corbet, Cyril; Page, Adeline; Ataman-Önal, Yasemin; Choquet-Kastylevsky, Geneviève; Fliniaux, Ingrid; Bourhis, Xuefen Le; Toillon, Robert‐Alain; Bradshaw, Ralph A.; Hondermarck, Hubert

doi:10.1074/jbc.m110.211714

Cited by 73 publications

(85 citation statements)

References 35 publications

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“…As described above, breast cancers express and respond to NGF, and therefore the discovery that proNGF is secreted by tumor cells was not overly surprising (Demont et al ., 2012). However the determination that it stimulates their migration/invasion through an autocrine loop mediated by TrkA and sortilin was unexpected.…”

Section: Prongf As An Active Growth Factormentioning

confidence: 99%

“…In addition, a comparison between proNGF levels and clinicopathological parameters revealed a correlation with lymph node invasion. In invasive ductal carcinomas, which represent the majority of breast cancers, there was no correlation with histological grade, tumor value, axillary lymph node status, age and presence of estrogen receptors, although a statistically significant association was obtained between the quantity of proNGF and lymph node invasion, suggesting a link to metastasis (Demont et al ., 2012). Indeed, proNGF may serve as a biomarker of metastasis and possibly as a therapeutic target in breast cancer.…”

Section: Prongf As An Active Growth Factormentioning

confidence: 99%

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NGF and ProNGF: Regulation of neuronal and neoplastic responses through receptor signaling

Bradshaw

Pundavela

Biarc

et al. 2015

Advances in Biological Regulation

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102

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Nerve growth factor (NGF) and its precursor (proNGF) are primarily considered as regulators of neuronal function that induce their responses via the tyrosine kinase receptor TrkA and the pan-neurotrophin receptor p75NTR. It has been generally held that NGF exerts its effects primarily through TrkA, inducing a cascade of tyrosine kinase-initiated responses, while proNGF binds more strongly to p75NTR. When this latter entity interacts with a third receptor, sortilin, apoptotic responses are induced in contrast to the survival/differentiation associated with the other two. Recent studies have outlined portions of the downstream phosphoproteome of TrkA in the neuronal PC12 cells and have clarified the contribution of individual docking sites in the TrkA endodomain. The patterns observed showed a similarity with the profile induced by the epidermal growth factor receptor, which is extensively associated with oncogenesis. Indeed, as with other neurotrophic factors, the distribution of TrkA and p75NTR is not limited to neuronal tissue, thus providing an array of targets outside the nervous systems. One such source is breast cancer cells, in which NGF and proNGF stimulate breast cancer cell survival/growth and enhance cell invasion, respectively. This latter activity is exerted via TrkA (as opposed to p75NTR) in conjunction with sortilin. Another tissue overexpressing proNGF is prostate cancer and here the ability of cancer cells to induce neuritogenesis has been implicated in cancer progression. These studies show that the non-neuronal functions of proNGF/NGF are likely integrated with their neuronal activities and point to the clinical utility of these growth factors and their receptors as biomarkers and therapeutic targets for metastasis and cancer pain.

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Section: Prongf As An Active Growth Factormentioning

confidence: 99%

Section: Prongf As An Active Growth Factormentioning

confidence: 99%

NGF and ProNGF: Regulation of neuronal and neoplastic responses through receptor signaling

Bradshaw

Pundavela

Biarc

et al. 2015

Advances in Biological Regulation

Self Cite

102

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“…This has been particularly well described for neurotrophins in breast cancer (22). For instance, NGF and proNGF are expressed in breast cancer and stimulate tumor cell growth and invasion (23,24), including the stem cell compartment (25). In prostate cancer, changes in the expression of NGF and its Trk receptor contribute to tumor cell growth and dissemination through a variety of kinasebased signaling pathways, and the inhibition of Trk receptors decreases the growth of prostatic cancer cells (26).…”

Section: Potential Antineurogenic Therapies In Cancermentioning

confidence: 99%

Nerve–Cancer Cell Cross-talk: A Novel Promoter of Tumor Progression

et al. 2015

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Recent studies have revealed the essential role played by nerves in tumor progression. Nerves have been shown to infiltrate the tumor microenvironment and actively stimulate cancer cell growth and dissemination. This mechanism involves the release of neurotransmitters, such as catecholamines and acetylcholine, directly into the vicinity of cancer and stromal cells to activate corresponding membrane receptors. Conversely, the secretion of neurotrophic growth factors by cancer cells drives the outgrowth of nerves in solid tumors. This reciprocal interaction between nerves and cancer cells provides new insights into the cellular and molecular bases of tumorigenesis and points to the potential utility of antineurogenic therapies. This review will discuss our evolving understanding of the cross-talk between nerves and cancer cells. Cancer Res; 75(9);

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“…We have previously described another function of sortilin, as a crucial protein to form a complex with two receptors containing a tyrosine kinase domain, TrkB and EGFR, in lung cancer [48]. Sortilin complexed with TrkA, another tyrosine kinase receptor for NGF, was also identified in breast cancer, promoting cell invasion through pro-NGF binding to this complex [49]. Similar results were reported in melanoma, expressing Trks, p75 NTR and sortilin, wherein cell migration and invasion induced by pro-NGF were depending on p75 NTR [50].…”

Section: Discussionmentioning

confidence: 99%

p75 neurotrophin receptor and pro-BDNF promote cell survival and migration in clear cell renal cell carcinoma

et al. 2016

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p75NTR, a member of TNF receptor family, is the low affinity receptor common to several mature neurotrophins and the high affinity receptor for pro-neurotrophins. Brain-Derived Neurotrophic Factor (BDNF), a member of neurotrophin family has been described to play an important role in development and progression of several cancers, through its binding to a high affinity tyrosine kinase receptor B (TrkB) and/or p75NTR. However, the functions of these two receptors in renal cell carcinoma (RCC) have never been investigated. An overexpression of p75NTR, pro-BDNF, and to a lesser extent for TrkB and sortilin, was detected by immunohistochemistry in a cohort of 83 clear cell RCC tumors. p75NTR, mainly expressed in tumor tissues, was significantly associated with higher Fuhrman grade in multivariate analysis. In two derived-RCC lines, 786-O and ACHN cells, we demonstrated that pro-BDNF induced cell survival and migration, through p75NTR as provided by p75NTR RNA silencing or blocking anti-p75NTR antibody. This mechanism is independent of TrkB activation as demonstrated by k252a, a tyrosine kinase inhibitor for Trk neurotrophin receptors. Taken together, these data highlight for the first time an important role for p75NTR in renal cancer and indicate a putative novel target therapy in RCC.

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Pro-nerve Growth Factor Induces Autocrine Stimulation of Breast Cancer Cell Invasion through Tropomyosin-related Kinase A (TrkA) and Sortilin Protein

Cited by 73 publications

References 35 publications

NGF and ProNGF: Regulation of neuronal and neoplastic responses through receptor signaling

NGF and ProNGF: Regulation of neuronal and neoplastic responses through receptor signaling

Nerve–Cancer Cell Cross-talk: A Novel Promoter of Tumor Progression

p75 neurotrophin receptor and pro-BDNF promote cell survival and migration in clear cell renal cell carcinoma

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