Your search keyword '"Gertler, Frank"' showing total 12 results

1. Lamellipodin-Deficient Mice: A Model of Rectal Carcinoma

Author

Massachusetts Institute of Technology. Department of Biological Engineering, Massachusetts Institute of Technology. Division of Comparative Medicine, Koch Institute for Integrative Cancer Research at MIT, Miller, Cassandra L., Muthupalani, Sureshkumar, Shen, Zeli, Drees, Frauke, Ge, Zhongming, Feng, Yan, Gong, Guanyu, Gertler, Frank, Fox, James G, Chen, Xiaowei, Nagar, Karan K., Wang, Timothy C., Massachusetts Institute of Technology. Department of Biological Engineering, Massachusetts Institute of Technology. Division of Comparative Medicine, Koch Institute for Integrative Cancer Research at MIT, Miller, Cassandra L., Muthupalani, Sureshkumar, Shen, Zeli, Drees, Frauke, Ge, Zhongming, Feng, Yan, Gong, Guanyu, Gertler, Frank, Fox, James G, Chen, Xiaowei, Nagar, Karan K., and Wang, Timothy C.

Abstract

During a survey of clinical rectal prolapse (RP) cases in the mouse population at MIT animal research facilities, a high incidence of RP in the lamellipodin knock-out strain, C57BL/6-Raph1[superscript tm1Fbg] (Lpd[superscript -/-]) was documented. Upon further investigation, the Lpd[superscript -/-] colony was found to be infected with multiple endemic enterohepatic Helicobacter species (EHS). Lpd[superscript -/-] mice, a transgenic mouse strain produced at MIT, have not previously shown a distinct immune phenotype and are not highly susceptible to other opportunistic infections. Predominantly male Lpd[superscript -/-] mice with RP exhibited lesions consistent with invasive rectal carcinoma concomitant to clinically evident RP. Multiple inflammatory cytokines, CD11b+Gr1+ myeloid-derived suppressor cell (MDSC) populations, and epithelial cells positive for a DNA damage biomarker, H2AX, were elevated in affected tissue, supporting their role in the neoplastic process. An evaluation of Lpd[superscript -/-] mice with RP compared to EHS-infected, but clinically normal (CN) Lpd[superscript -/-] animals indicated that all of these mice exhibit some degree of lower bowel inflammation; however, mice with prolapses had significantly higher degree of focal lesions at the colo-rectal junction. When Helicobacter spp. infections were eliminated in Lpd[superscript -/-] mice by embryo transfer rederivation, the disease phenotype was abrogated, implicating EHS as a contributing factor in the development of rectal carcinoma. Here we describe lesions in Lpd[superscript -/-] male mice consistent with a focal inflammation-induced neoplastic transformation and propose this strain as a mouse model of rectal carcinoma., United States. National Institutes of Health (T32-OD010978), United States. National Institutes of Health (R01-OD011141), United States. National Institutes of Health (P30-ES002109), Massachusetts Institute of Technology. Ludwig Center for Molecular Oncology (U54- CA114462), National Cancer Institute (U.S.) (P30-CA14051)

Published

2017

2. Eps8 Regulates Axonal Filopodia in Hippocampal Neurons in Response to Brain-Derived Neurotrophic Factor (BDNF)

Author

Menna, Elisabetta, Disanza, Andrea, Cagnoli, Cinzia, Schenk, Ursula, Gelsomino, Giuliana, Frittoli, Emanuela, Hertzog, Maud, Offenhauser, Nina, Sawallisch, Corinna, Kreienkamp, Hans-Jürgen, Gertler, Frank B., Di Fiore, Pier Paolo, Scita, Giorgio, and Matteoli, Michela

Subjects

nervous system, Cell Biology/Cytoskeleton, Cell Biology/Neuronal Signaling Mechanisms, Neuroscience/Neuronal and Glial Cell Biology, education, Neuroscience/Neuronal Signaling Mechanisms, macromolecular substances, Cell Biology/Cell Signaling, Research Article

Abstract

A novel signaling cascade controlling actin polymerization in response to extracellular signals regulates filopodia formation and likely also neuronal synapse formation., The regulation of filopodia plays a crucial role during neuronal development and synaptogenesis. Axonal filopodia, which are known to originate presynaptic specializations, are regulated in response to neurotrophic factors. The structural components of filopodia are actin filaments, whose dynamics and organization are controlled by ensembles of actin-binding proteins. How neurotrophic factors regulate these latter proteins remains, however, poorly defined. Here, using a combination of mouse genetic, biochemical, and cell biological assays, we show that genetic removal of Eps8, an actin-binding and regulatory protein enriched in the growth cones and developing processes of neurons, significantly augments the number and density of vasodilator-stimulated phosphoprotein (VASP)-dependent axonal filopodia. The reintroduction of Eps8 wild type (WT), but not an Eps8 capping-defective mutant, into primary hippocampal neurons restored axonal filopodia to WT levels. We further show that the actin barbed-end capping activity of Eps8 is inhibited by brain-derived neurotrophic factor (BDNF) treatment through MAPK-dependent phosphorylation of Eps8 residues S624 and T628. Additionally, an Eps8 mutant, impaired in the MAPK target sites (S624A/T628A), displays increased association to actin-rich structures, is resistant to BDNF-mediated release from microfilaments, and inhibits BDNF-induced filopodia. The opposite is observed for a phosphomimetic Eps8 (S624E/T628E) mutant. Thus, collectively, our data identify Eps8 as a critical capping protein in the regulation of axonal filopodia and delineate a molecular pathway by which BDNF, through MAPK-dependent phosphorylation of Eps8, stimulates axonal filopodia formation, a process with crucial impacts on neuronal development and synapse formation., Author Summary Neurons communicate with each other via specialized cell–cell junctions called synapses. The proper formation of synapses (“synaptogenesis”) is crucial to the development of the nervous system, but the molecular pathways that regulate this process are not fully understood. External cues, such as brain-derived neurotrophic factor (BDNF), trigger synaptogenesis by promoting the formation of axonal filopodia, thin extensions projecting outward from a growing axon. Filopodia are formed by elongation of actin filaments, a process that is regulated by a complex set of actin-binding proteins. Here, we reveal a novel molecular circuit underlying BDNF-stimulated filopodia formation through the regulated inhibition of actin-capping factor activity. We show that the actin-capping protein Eps8 down-regulates axonal filopodia formation in neurons in the absence of neurotrophic factors. In contrast, in the presence of BDNF, the kinase MAPK becomes activated and phosphorylates Eps8, leading to inhibition of its actin-capping function and stimulation of filopodia formation. Our study, therefore, identifies actin-capping factor inhibition as a critical step in axonal filopodia formation and likely in new synapse formation.

Published

2009

3. Peptide Array X-Linking (PAX): A New Peptide-Protein Identification Approach

Author

David H. Koch Institute for Integrative Cancer Research at MIT, Massachusetts Institute of Technology. Department of Biology, Gertler, Frank, Okada, Hirokazu, Uezu, Akiyoshi, Soderblom, Erik J., Moseley, M. Arthur, III, Soderling, Scott H., David H. Koch Institute for Integrative Cancer Research at MIT, Massachusetts Institute of Technology. Department of Biology, Gertler, Frank, Okada, Hirokazu, Uezu, Akiyoshi, Soderblom, Erik J., Moseley, M. Arthur, III, and Soderling, Scott H.

Abstract

Many protein interaction domains bind short peptides based on canonical sequence consensus motifs. Here we report the development of a peptide array-based proteomics tool to identify proteins directly interacting with ligand peptides from cell lysates. Array-formatted bait peptides containing an amino acid-derived cross-linker are photo-induced to crosslink with interacting proteins from lysates of interest. Indirect associations are removed by high stringency washes under denaturing conditions. Covalently trapped proteins are subsequently identified by LC-MS/MS and screened by cluster analysis and domain scanning. We apply this methodology to peptides with different proline-containing consensus sequences and show successful identifications from brain lysates of known and novel proteins containing polyproline motif-binding domains such as EH, EVH1, SH3, WW domains. These results suggest the capacity of arrayed peptide ligands to capture and subsequently identify proteins by mass spectrometry is relatively broad and robust. Additionally, the approach is rapid and applicable to cell or tissue fractions from any source, making the approach a flexible tool for initial protein-protein interaction discovery., National Institutes of Health (U.S.) (Grant R21-CA-140030-01)

Published

2012

4. Peptide Array X-Linking (PAX): A New Peptide-Protein Identification Approach

Author

Massachusetts Institute of Technology. Department of Biology, Koch Institute for Integrative Cancer Research at MIT, Gertler, Frank, Okada, Hirokazu, Uezu, Akiyoshi, Soderblom, Erik J., Moseley, M. Arthur, III, Soderling, Scott H., Massachusetts Institute of Technology. Department of Biology, Koch Institute for Integrative Cancer Research at MIT, Gertler, Frank, Okada, Hirokazu, Uezu, Akiyoshi, Soderblom, Erik J., Moseley, M. Arthur, III, and Soderling, Scott H.

Abstract

Many protein interaction domains bind short peptides based on canonical sequence consensus motifs. Here we report the development of a peptide array-based proteomics tool to identify proteins directly interacting with ligand peptides from cell lysates. Array-formatted bait peptides containing an amino acid-derived cross-linker are photo-induced to crosslink with interacting proteins from lysates of interest. Indirect associations are removed by high stringency washes under denaturing conditions. Covalently trapped proteins are subsequently identified by LC-MS/MS and screened by cluster analysis and domain scanning. We apply this methodology to peptides with different proline-containing consensus sequences and show successful identifications from brain lysates of known and novel proteins containing polyproline motif-binding domains such as EH, EVH1, SH3, WW domains. These results suggest the capacity of arrayed peptide ligands to capture and subsequently identify proteins by mass spectrometry is relatively broad and robust. Additionally, the approach is rapid and applicable to cell or tissue fractions from any source, making the approach a flexible tool for initial protein-protein interaction discovery., National Institutes of Health (U.S.) (Grant R21-CA-140030-01)

Published

2012

5. An EMT-Driven Alternative Splicing Program Occurs in Human Breast Cancer and Modulates Cellular Phenotype

Author

David H. Koch Institute for Integrative Cancer Research at MIT, Massachusetts Institute of Technology. Computational and Systems Biology Program, Massachusetts Institute of Technology. Department of Biological Engineering, Massachusetts Institute of Technology. Department of Biology, Gertler, Frank, Shapiro, Irina M., Cheng, Albert W., Flytzanis, Nicholas C., Balsamo, Michele, Burge, Christopher B., Condeelis, John S., Oktay, Maja H., David H. Koch Institute for Integrative Cancer Research at MIT, Massachusetts Institute of Technology. Computational and Systems Biology Program, Massachusetts Institute of Technology. Department of Biological Engineering, Massachusetts Institute of Technology. Department of Biology, Gertler, Frank, Shapiro, Irina M., Cheng, Albert W., Flytzanis, Nicholas C., Balsamo, Michele, Burge, Christopher B., Condeelis, John S., and Oktay, Maja H.

Abstract

Epithelial-mesenchymal transition (EMT), a mechanism important for embryonic development, plays a critical role during malignant transformation. While much is known about transcriptional regulation of EMT, alternative splicing of several genes has also been correlated with EMT progression, but the extent of splicing changes and their contributions to the morphological conversion accompanying EMT have not been investigated comprehensively. Using an established cell culture model and RNA–Seq analyses, we determined an alternative splicing signature for EMT. Genes encoding key drivers of EMT–dependent changes in cell phenotype, such as actin cytoskeleton remodeling, regulation of cell–cell junction formation, and regulation of cell migration, were enriched among EMT–associated alternatively splicing events. Our analysis suggested that most EMT–associated alternative splicing events are regulated by one or more members of the RBFOX, MBNL, CELF, hnRNP, or ESRP classes of splicing factors. The EMT alternative splicing signature was confirmed in human breast cancer cell lines, which could be classified into basal and luminal subtypes based exclusively on their EMT–associated splicing pattern. Expression of EMT–associated alternative mRNA transcripts was also observed in primary breast cancer samples, indicating that EMT–dependent splicing changes occur commonly in human tumors. The functional significance of EMT–associated alternative splicing was tested by expression of the epithelial-specific splicing factor ESRP1 or by depletion of RBFOX2 in mesenchymal cells, both of which elicited significant changes in cell morphology and motility towards an epithelial phenotype, suggesting that splicing regulation alone can drive critical aspects of EMT–associated phenotypic changes. The molecular description obtained here may aid in the development of new diagnostic and prognostic markers for analysis of breast cancer progression., National Institutes of Health (U.S.) (R01-HG002439), National Science Foundation (U.S.) (equipment grant), National Institutes of Health (U.S.) (Integrative Cancer Biology Program Grant U54-CA112967), David H. Koch Institute for Integrative Cancer Research at MIT (Ludwig Center for Metastasis Research), David H. Koch Institute for Integrative Cancer Research at MIT, Massachusetts Institute of Technology (Croucher Scholarship), Massachusetts Institute of Technology (Ludwig Fund postdoctoral fellowship), National Institutes of Health (U.S.) (NIH CA100324), National Institutes of Health (U.S.) (AECC9526-5267)

Published

2011

6. Eps8 Regulates Axonal Filopodia in Hippocampal Neurons in Response to Brain-Derived Neurotrophic Factor (BDNF)

Author

Massachusetts Institute of Technology. Department of Biology, Gertler, Frank, Matteoli, Michela, Scita, Giorgio, Di Fiore, Pier Paolo, Kreienkamp, Hans-Jürgen, Sawallisch, Corinna, Offenhauser, Nina, Hertzog, Maud, Frittoli, Emanuela, Gelsomino, Giuliana, Schenk, Ursula, Cagnoli, Cinzia, Disanza, Andrea, Menna, Elisabetta, Massachusetts Institute of Technology. Department of Biology, Gertler, Frank, Matteoli, Michela, Scita, Giorgio, Di Fiore, Pier Paolo, Kreienkamp, Hans-Jürgen, Sawallisch, Corinna, Offenhauser, Nina, Hertzog, Maud, Frittoli, Emanuela, Gelsomino, Giuliana, Schenk, Ursula, Cagnoli, Cinzia, Disanza, Andrea, and Menna, Elisabetta

Abstract

The regulation of filopodia plays a crucial role during neuronal development and synaptogenesis. Axonal filopodia, which are known to originate presynaptic specializations, are regulated in response to neurotrophic factors. The structural components of filopodia are actin filaments, whose dynamics and organization are controlled by ensembles of actin-binding proteins. How neurotrophic factors regulate these latter proteins remains, however, poorly defined. Here, using a combination of mouse genetic, biochemical, and cell biological assays, we show that genetic removal of Eps8, an actin-binding and regulatory protein enriched in the growth cones and developing processes of neurons, significantly augments the number and density of vasodilator-stimulated phosphoprotein (VASP)-dependent axonal filopodia. The reintroduction of Eps8 wild type (WT), but not an Eps8 capping-defective mutant, into primary hippocampal neurons restored axonal filopodia to WT levels. We further show that the actin barbed-end capping activity of Eps8 is inhibited by brain-derived neurotrophic factor (BDNF) treatment through MAPK-dependent phosphorylation of Eps8 residues S624 and T628. Additionally, an Eps8 mutant, impaired in the MAPK target sites (S624A/T628A), displays increased association to actin-rich structures, is resistant to BDNF-mediated release from microfilaments, and inhibits BDNF-induced filopodia. The opposite is observed for a phosphomimetic Eps8 (S624E/T628E) mutant. Thus, collectively, our data identify Eps8 as a critical capping protein in the regulation of axonal filopodia and delineate a molecular pathway by which BDNF, through MAPK-dependent phosphorylation of Eps8, stimulates axonal filopodia formation, a process with crucial impacts on neuronal development and synapse formation.

Published

2010

7. Lamellipodin-Deficient Mice: A Model of Rectal Carcinoma.

Author

Miller, Cassandra L., Muthupalani, Sureshkumar, Shen, Zeli, Drees, Frauke, Ge, Zhongming, Feng, Yan, Chen, Xiaowei, Gong, Guanyu, Nagar, Karan K., Wang, Timothy C., Gertler, Frank B., and Fox, James G.

Subjects

RECTAL cancer, RECTAL prolapse, PHENOTYPES, BIOMARKERS, DNA damage, LABORATORY mice

Abstract

During a survey of clinical rectal prolapse (RP) cases in the mouse population at MIT animal research facilities, a high incidence of RP in the lamellipodin knock-out strain, C57BL/6-Raph1tm1Fbg (Lpd-/-) was documented. Upon further investigation, the Lpd-/- colony was found to be infected with multiple endemic enterohepatic Helicobacter species (EHS). Lpd-/- mice, a transgenic mouse strain produced at MIT, have not previously shown a distinct immune phenotype and are not highly susceptible to other opportunistic infections. Predominantly male Lpd-/- mice with RP exhibited lesions consistent with invasive rectal carcinoma concomitant to clinically evident RP. Multiple inflammatory cytokines, CD11b+Gr1+ myeloid-derived suppressor cell (MDSC) populations, and epithelial cells positive for a DNA damage biomarker, H2AX, were elevated in affected tissue, supporting their role in the neoplastic process. An evaluation of Lpd-/- mice with RP compared to EHS-infected, but clinically normal (CN) Lpd-/- animals indicated that all of these mice exhibit some degree of lower bowel inflammation; however, mice with prolapses had significantly higher degree of focal lesions at the colo-rectal junction. When Helicobacter spp. infections were eliminated in Lpd-/- mice by embryo transfer rederivation, the disease phenotype was abrogated, implicating EHS as a contributing factor in the development of rectal carcinoma. Here we describe lesions in Lpd-/- male mice consistent with a focal inflammation-induced neoplastic transformation and propose this strain as a mouse model of rectal carcinoma. [ABSTRACT FROM AUTHOR]

Published

2016

8. Peptide Array X-Linking (PAX): A New Peptide-Protein Identification Approach.

Author

Okada, Hirokazu, Uezu, Akiyoshi, Soderblom, Erik J., Moseley, III., M. Arthur, Gertler, Frank B., and Soderling, Scott H.

Subjects

PROTEIN-protein interactions, PEPTIDES, PROTEOMICS, LIGANDS (Biochemistry), POLYPROLINE, PAX (Osculatory), MASS spectrometry

Abstract

Many protein interaction domains bind short peptides based on canonical sequence consensus motifs. Here we report the development of a peptide array-based proteomics tool to identify proteins directly interacting with ligand peptides from cell lysates. Array-formatted bait peptides containing an amino acid-derived cross-linker are photo-induced to crosslink with interacting proteins from lysates of interest. Indirect associations are removed by high stringency washes under denaturing conditions. Covalently trapped proteins are subsequently identified by LC-MS/MS and screened by cluster analysis and domain scanning. We apply this methodology to peptides with different proline-containing consensus sequences and show successful identifications from brain lysates of known and novel proteins containing polyproline motif-binding domains such as EH, EVH1, SH3, WW domains. These results suggest the capacity of arrayed peptide ligands to capture and subsequently identify proteins by mass spectrometry is relatively broad and robust. Additionally, the approach is rapid and applicable to cell or tissue fractions from any source, making the approach a flexible tool for initial protein-protein interaction discovery. [ABSTRACT FROM AUTHOR]

Published

2012

9. An EMT--Driven Alternative Splicing Program Occurs in Human Breast Cancer and Modulates Cellular Phenotype.

Author

Shapiro, Irina M., Cheng, Albert W., Flytzanis, Nicholas C., Balsamo, Michele, Condeelis, John S., Oktay, Maja H., Burge, Christopher B., and Gertler, Frank B.

Subjects

BREAST cancer, PHENOTYPES, EMBRYOLOGY, TRANSCRIPTION factors, CANCER invasiveness, EPITHELIAL cells, RNA splicing

Abstract

Epithelial-mesenchymal transition (EMT), a mechanism important for embryonic development, plays a critical role during malignant transformation. While much is known about transcriptional regulation of EMT, alternative splicing of several genes has also been correlated with EMT progression, but the extent of splicing changes and their contributions to the morphological conversion accompanying EMT have not been investigated comprehensively. Using an established cell culture model and RNA--Seq analyses, we determined an alternative splicing signature for EMT. Genes encoding key drivers of EMT--dependent changes in cell phenotype, such as actin cytoskeleton remodeling, regulation of cell--cell junction formation, and regulation of cell migration, were enriched among EMT--associated alternatively splicing events. Our analysis suggested that most EMT--associated alternative splicing events are regulated by one or more members of the RBFOX, MBNL, CELF, hnRNP, or ESRP classes of splicing factors. The EMT alternative splicing signature was confirmed in human breast cancer cell lines, which could be classified into basal and luminal subtypes based exclusively on their EMT--associated splicing pattern. Expression of EMT--associated alternative mRNA transcripts was also observed in primary breast cancer samples, indicating that EMT--dependent splicing changes occur commonly in human tumors. The functional significance of EMT--associated alternative splicing was tested by expression of the epithelial-specific splicing factor ESRP1 or by depletion of RBFOX2 in mesenchymal cells, both of which elicited significant changes in cell morphology and motility towards an epithelial phenotype, suggesting that splicing regulation alone can drive critical aspects of EMT--associated phenotypic changes. The molecular description obtained here may aid in the development of new diagnostic and prognostic markers for analysis of breast cancer progression. [ABSTRACT FROM AUTHOR]

Published

2011

10. Emergence of Large-Scale Cell Morphology and Movement from Local Actin Filament Growth Dynamics.

Author

Lacayo, Catherine I., Pincus, Zachary, VanDuijn, Martijn M., Wilson, Cyrus A., Fletcher, Daniel A., Gertler, Frank B., Mogilner, Alex, and Theriot, Julie A.

Subjects

CELLS, ACTIN, CELL migration, PROTEINS, CYTOSKELETON, VASODILATORS

Abstract

Mathematical modeling predicts global modifications of the shape and behavior of migrating cells from knowledge of detailed multiscale protein interactions. [ABSTRACT FROM AUTHOR]

Published

2007

11. Correction: Eps8 Regulates Axonal Filopodia in Hippocampal Neurons in Response to Brain-Derived Neurotrophic Factor (BDNF).

Author

Menna, Elisabetta, Disanza, Andrea, Cagnoli, Cinzia, Schenk, Ursula, Gelsomino, Giuliana, Frittoli, Emanuela, Hertzog, Maud, Offenhauser, Nina, Sawallisch, Corinna, Kreienkamp, Hans-Jürgen, Gertler, Frank B., Di Fiore, Pier Paolo, Scita, Giorgio, and Matteoli, Michela

Subjects

NEURONS, LAMELLIPODIA

Abstract

A correction to the article "Eps8 Regulates Axonal Filopodia in Hippocampal Neurons in Response to Brain-Derived Neurotrophic Factor (BDNF)" by Elisabetta Menna that was published in the previous issue.

Published

2015

12. Eps8 Regulates Axonal Filopodia in Hippocampal Neurons in Response to Brain-Derived Neurotrophic Factor (BDNF)

Author

Andrea Disanza, Cinzia Cagnoli, Corinna Sawallisch, Michela Matteoli, Pier Paolo Di Fiore, Ursula Schenk, Emanuela Frittoli, Hans Jürgen Kreienkamp, Frank B. Gertler, Giorgio Scita, Elisabetta Menna, Nina Offenhäuser, Giuliana Gelsomino, Maud Hertzog, Massachusetts Institute of Technology. Department of Biology, and Gertler, Frank

Subjects

Brain-derived neurotrophic factor, 0303 health sciences, General Immunology and Microbiology, QH301-705.5, General Neuroscience, Synaptogenesis, macromolecular substances, Biology, SRGAP2, General Biochemistry, Genetics and Molecular Biology, Cell biology, 03 medical and health sciences, 0302 clinical medicine, nervous system, Neurotrophic factors, Fimbrin, Pseudopodia, Biology (General), General Agricultural and Biological Sciences, Growth cone, Filopodia, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

The regulation of filopodia plays a crucial role during neuronal development and synaptogenesis. Axonal filopodia, which are known to originate presynaptic specializations, are regulated in response to neurotrophic factors. The structural components of filopodia are actin filaments, whose dynamics and organization are controlled by ensembles of actin-binding proteins. How neurotrophic factors regulate these latter proteins remains, however, poorly defined. Here, using a combination of mouse genetic, biochemical, and cell biological assays, we show that genetic removal of Eps8, an actin-binding and regulatory protein enriched in the growth cones and developing processes of neurons, significantly augments the number and density of vasodilator-stimulated phosphoprotein (VASP)-dependent axonal filopodia. The reintroduction of Eps8 wild type (WT), but not an Eps8 capping-defective mutant, into primary hippocampal neurons restored axonal filopodia to WT levels. We further show that the actin barbed-end capping activity of Eps8 is inhibited by brain-derived neurotrophic factor (BDNF) treatment through MAPK-dependent phosphorylation of Eps8 residues S624 and T628. Additionally, an Eps8 mutant, impaired in the MAPK target sites (S624A/T628A), displays increased association to actin-rich structures, is resistant to BDNF-mediated release from microfilaments, and inhibits BDNF-induced filopodia. The opposite is observed for a phosphomimetic Eps8 (S624E/T628E) mutant. Thus, collectively, our data identify Eps8 as a critical capping protein in the regulation of axonal filopodia and delineate a molecular pathway by which BDNF, through MAPK-dependent phosphorylation of Eps8, stimulates axonal filopodia formation, a process with crucial impacts on neuronal development and synapse formation.

Published

2009