Heregulin-dependent regulation of HER2/neu oncogenic signaling by heterodimerization with HER3.

Wallasch, Christian; Weiß, Florian; Niederfellner, Gerhard; Jallal, Bahija; Issing, W. J.; Ullrich, Axel

doi:10.1002/j.1460-2075.1995.tb00101.x

Cited by 388 publications

(312 citation statements)

References 55 publications

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“…Consistent with this notion, neuregulin-mediated proliferation of keratinocytes (Danilenko et al, 1995;Marikovsky et al, 1995), mammary cells (Holmes et al, 1992) and Schwann cells correlates with coexpression of ErbB-2 together with ErB-3, rather than with ErbB-4. Thus, ErbB-3 action may be restricted to cell proliferation, in agreement with the potent mitogenic activity of this receptor in normal (PinkasKramarski et al, 1996) and in tumor cells (Alimandi et al, 1995;Wallasch et al, 1995). However, fatedetermining processes, that do not involve mitosis, may be associated with ErbB-4, whose signaling capacity is rather limited.…”

Section: Inhibition Of Neuronal DI Erentiation By Ndfmentioning

confidence: 70%

Differential expression of NDF/neuregulin receptors ErbB-3 and ErbB-4 and involvement in inhibition of neuronal differentiation

et al. 1997

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Two receptor tyrosine kinases, ErB-3 and ErbB-4, mediate signaling by Neu di erentiation factors (NDFs, also called neuregulins), while ErbB-1 and ErbB-2 serve as co-receptors. We show that the two NDF/neuregulin receptors di er in spatial and temporal expression patterns: The kinase-defective receptor, ErbB-3, is expressed primarily in epithelial layers of various organs, in the peripheral nervous system, and in adult brain, whereas ErbB-4 is restricted to the developing central nervous system and to the embryonic heart. An example of alternating expression of the two receptors is provided by the developing cerebellum: During postnatal cerebellar development, ErbB-4 expression slightly decreases along with a decline in NDF transcription, whereas ErbB-3 expression commences after the peak of neurogenesis. To study functional di erences, we established primary brain cultures and found that ErbB-3 was expressed only in oligodendrocytes, whereas ErbB-4 expression was shared by oligodendrocytes, astrocytes and neurons. Blocking the action of endogenous NDF in vitro, by using a soluble form of ErbB-4, accelerated neurite outgrowth in both primary cultures and in neuronal-type cultures of the P19 teratocarcinoma, suggesting an inhibitory e ect of NDF on neural di erentiation. Apparently, ErbB-3 is associated with proliferation of P19 cells, whereas ErbB-4 correlates with a di erentiated phenotype. We conclude that the two NDF receptors play distinct, rather than redundant, developmental and physiological roles.

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Section: Inhibition Of Neuronal DI Erentiation By Ndfmentioning

confidence: 70%

Differential expression of NDF/neuregulin receptors ErbB-3 and ErbB-4 and involvement in inhibition of neuronal differentiation

et al. 1997

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“…These data suggest that c-erbB3, and possibly c-erbB4, are involved in aspects of tumour cell di erentiation, rather than in directing cellular growth patterns. Furthermore, although our study does not address the transforming ability of c-erbB3 (or cerbB4), which has previously been shown to be greatly enhanced by the co-expression with c-erbB2 or EGFR in ®broblasts (Alimandi et al, 1995;Wallasch et al, 1995), the detection of c-erbB3 (mRNA and protein) in endocrine sensitive cancers at levels equivalent to those seen in normal breast tissue (albeit cancer associated) would not support a direct transforming role for cerbB3.…”

Section: Discussionmentioning

confidence: 99%

c-erbB3 and c-erbB4 expression is a feature of the endocrine responsive phenotype in clinical breast cancer

et al. 1998

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We examined c-erbB3 and c-erbB4 mRNA expression in 47 primary breast cancer samples by simultaneous RT ± PCR and have investigated correlations between these parameters and the expression of both ER and EGFR mRNA and protein as measured by RT ± PCR and ICA and with Ki67 immunostaining. A direct association was found between c-erbB3 and c-erbB4 mRNA and ER marker status measured by either RT ± PCR (c-erbB3 P=0.0003; c-erbB4 P=0.02) or ICA (c-erbB-3 P=0.002; c-erbB4 P=0.01). Inverse associations were seen between c-erbB3 and c-erbB4 mRNA marker status and EGFR membrane protein (c-erbB3: P=0.003; cerbB4: P=0.003) and mRNA (c-erbB4: P=0.009) status. These associations were reinforced by Spearman Rank Correlation Tests. A signi®cant relationship was seen between Ki67 and c-erbB4 mRNA status and level. Measurements of c-erbB3 protein levels in tumour samples removed from a further 89 patients of known response to endocrine therapy: (i) con®rmed the relationship between c-erbB3 and ER and (ii) identi®ed that patients whose ER positive tumours expressed high levels of c-erbB3 were most likely to bene®t from endocrine measures. A non-signi®cant trend was recorded between c-erbB3 levels and Ki67 immunostaining. These results clearly demonstrate that increased c-erbB3 and c-erbB4 expression appears to be associated with the prognostically-favourable ER phenotype.

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“…ErbB2 by itself is not able to e ciently induce PI3-kinase activation (Peles et al, 1992), but when co-expressed with ErbB3, PI3-kinase activity is strongly increased. This is due to the e cient ErbB2-mediated transphosphorylation of ErbB3, which supplies phosphorylation sites for PI3-kinase (Wallasch et al, 1995).…”

Section: Discussionmentioning

confidence: 99%

Cross-talk between the proto-oncogenes Met and Ron

et al. 2000

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Heregulin-dependent regulation of HER2/neu oncogenic signaling by heterodimerization with HER3.

Cited by 388 publications

References 55 publications

Differential expression of NDF/neuregulin receptors ErbB-3 and ErbB-4 and involvement in inhibition of neuronal differentiation

Differential expression of NDF/neuregulin receptors ErbB-3 and ErbB-4 and involvement in inhibition of neuronal differentiation

c-erbB3 and c-erbB4 expression is a feature of the endocrine responsive phenotype in clinical breast cancer

Cross-talk between the proto-oncogenes Met and Ron

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