Spatial regulation of β-actin translation by Src-dependent phosphorylation of ZBP1

Hüttelmaier, Stefan; Zenklusen, Daniel; Lederer, Marcell; Dictenberg, Jason B.; Lorenz, Michael G.; Meng, Xiuhua; Bassell, Gary J.; Condeelis, John S.; Singer, Robert H.

doi:10.1038/nature04115

Cited by 553 publications

(665 citation statements)

References 23 publications

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“…In Xenopus, the ortholog Vg1-RBP is essential for the control of neuronal crest cell migration (Yaniv et al, 2003). In primary mammalian neurons as well as neuroblastoma cells, IMP1, also termed ZBP1 (zipcode-binding protein 1) regulates localized translation of the b-actin mRNA in growth cones and neurites supporting an important role of IMP proteins for guiding normal development and directing cell migration (Huttelmaier et al, 2005).…”

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confidence: 99%

“…Although additional target mRNAs of IMP1 are expected, solid evidence indicates that IMP1 is essential for the regulation of c-myc, bTrCP1 and CD44 mRNA turnover, but also facilitates translational control of the IGF-II and b-actin mRNAs (Nielsen et al, 1999;Lemm and Ross, 2002;Huttelmaier et al, 2005;Noubissi et al, 2006;Vikesaa et al, 2006). While by the regulation of IGF-II and c-myc expression IMP1 is expected to affect cell proliferation, growth and survival, the regulation of CD44 or b-actin expression via IMP1 is suggested to modulate cell adhesion, invadopodia formation and actin dynamics.…”

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confidence: 99%

“…To evaluate the role of IMP1 in ovarian carcinomas, phenotypic effects of aberrant IMP1 expression were analysed by small interfering RNA (siRNA)-mediated Immunostaining was performed on paraffin-embedded tissue sections, as described previously (Kobel et al, 2006), using a IMP1 (ZBP1)-directed antibody (Farina et al, 2003;Huttelmaier et al, 2005). Two slides per sample were immunostained together in two runs before the semiquantitative evaluation of the immunoreactivity by a pathologist (MK) blinded to the clinical data.…”

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confidence: 99%

“…(a) Cell viability was determined in ES-2 or OVCAR-3 cells at indicated time points after IMP1-directed siRNA transfection and normalization to cell viability in a population transfected with control siRNAs. The siRNAs used (one siRNA directed against IMP1 and one control siRNA) were as described previously (Huttelmaier et al, 2005). (b) ES-2 cell numbers were determined at indicated time points after siRNA transfection and normalization to cell numbers at 24 h post-transfection (100%).…”

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confidence: 99%

“…In (b), ES-2 cell numbers were determined post-transfection of indicated siRNAs and normalization to cell numbers 24 h post-transfection, set to 100%. The specific knockdown of IMP1 was determined by western blotting of OVCAR-3 and ES-2 cell lysates 72 h post-transfection with anti-vinculin (Sigma, Mu¨nchen, Germany), anti-tubulin (Sigma) and anti-IMP1 (ZBP1) (Farina et al, 2003), as described previously (Huttelmaier et al, 2005). Relative expression levels of indicated genes were determined by quantitative RT-PCR (d).…”

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Expression of the RNA-binding protein IMP1 correlates with poor prognosis in ovarian carcinoma

et al. 2007

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The IMP (IGFII mRNA-binding protein) family comprises a group of three RNA-binding proteins involved in the regulation of cytoplasmic mRNA-fate. Recent studies identified IMP proteins as oncofetal factors in various neoplasias, but knowledge of a potential role in ovarian carcinomas is still lacking. The immunohistochemical analysis of 107 ovarian carcinomas, 30 serous borderline tumors of the ovary and five normal ovaries revealed de novo synthesis of IMP1 in 69% of ovarian carcinomas. Elevated IMP1 expression was observed preferentially in high-grade and high-stage cases and was a significant prognostic indicator for reduced recurrence-free and overall survival. Phenotypic studies in ovarian carcinoma-derived ES-2 cells demonstrated that IMP1 knockdown affects proliferation and cell survival. Reduced proliferation was associated with decreased c-myc mRNA half-life, suggesting IMP1 as an oncogenic factor that is involved in promoting elevated proliferation by stabilizing the c-myc mRNA in ovarian carcinoma cells.

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Expression of the RNA-binding protein IMP1 correlates with poor prognosis in ovarian carcinoma

et al. 2007

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Spatially and temporally regulating translation via mRNA‐binding proteins in cellular and neuronal function

2017

Self Cite

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Edited by Wilhelm JustCoordinated regulation of mRNA localization and local translation are essential steps in cellular asymmetry and function. It is increasingly evident that mRNA-binding proteins play critical functions in controlling the fate of mRNA, including when and where translation occurs. In this review, we discuss the robust and complex roles that mRNA-binding proteins play in the regulation of local translation that impact cellular function in vertebrates. First, we discuss the role of local translation in cellular polarity and possible links to vertebrate development and patterning. Next, we discuss the expanding role for local protein synthesis in neuronal development and function, with special focus on how a number of neurological diseases have given us insight into the importance of translational regulation. Finally, we discuss the everincreasing set of tools to study regulated translation and how these tools will be vital in pushing forward and addressing the outstanding questions in the field.

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Moving messages in the developing brain—emerging roles for mRNA transport and local translation in neural stem cells

Pilaz

Silver

2017

FEBS Letters

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The mammalian cerebral cortex is a complex brain structure integral to our higher cognition. During embryonic cortical development, radial glial progenitors (RGCs) produce neurons and serve as physical structures for migrating neurons. Recent discoveries highlight new roles for RNA localization and local translation in RGCs, both at the cell body and at distal structures called basal endfeet. By implementing technologies from the field of RNA research to brain development, investigators can manipulate RNA-binding proteins as well as visualize single-molecule RNAs, live movement of mRNAs and their binding proteins, and translation. Going forward, these studies establish a framework for investigating how post-transcriptional RNA regulation helps shape RGC function and triggers neurodevelopmental diseases.

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Spatial regulation of β-actin translation by Src-dependent phosphorylation of ZBP1

Cited by 553 publications

References 23 publications

Expression of the RNA-binding protein IMP1 correlates with poor prognosis in ovarian carcinoma

Expression of the RNA-binding protein IMP1 correlates with poor prognosis in ovarian carcinoma

Spatially and temporally regulating translation via mRNA‐binding proteins in cellular and neuronal function

Moving messages in the developing brain—emerging roles for mRNA transport and local translation in neural stem cells

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