Your search keyword '"Alexander Korostylev"' showing total 5 results

1. A high-content small molecule screen identifies novel inducers of definitive endoderm

Author

Alexander Korostylev, Pallavi U. Mahaddalkar, Oliver Keminer, Kamyar Hadian, Kenji Schorpp, Philip Gribbon, and Heiko Lickert

Subjects

Rock inhibition, Fasudil, Pancreatic progenitors, Anterior definitive endoderm, Differentiations, Internal medicine, RC31-1245

Abstract

Objectives: Human embryonic stem cells (hESCs) and human induced pluripotent stem cells (hiPSCs) can generate any given cell type in the human body. One challenge for cell-replacement therapy is the efficient differentiation and expansion of large quantities of progenitor cells from pluripotent stem cells produced under good manufacturing practice (GMP). FOXA2 and SOX17 double positive definitive endoderm (DE) progenitor cells can give rise to all endoderm-derived cell types in the thymus, thyroid, lung, pancreas, liver, and gastrointestinal tract. FOXA2 is a pioneer transcription factor in DE differentiation that is also expressed and functionally required during pancreas development and islet cell homeostasis. Current differentiation protocols can successfully generate endoderm; however, generation of mature glucose-sensitive and insulin-secreting β-cells is still a challenge. As a result, it is of utmost importance to screen for small molecules that can improve DE and islet cell differentiation for cell-replacement therapy for diabetic patients. Methods: The aim of this study was to identify and validate small molecules that can induce DE differentiation and further enhance pancreatic progenitor differentiation. Therefore, we developed a large scale, high-content screen for testing a chemical library of 23,406 small molecules to identify compounds that induce FoxA2 in mouse embryonic stem cells (mESCs). Results: Based on our high-content screen algorithm, we selected 84 compounds that directed differentiation of mESCs towards the FoxA2 lineage. Strikingly, we identified ROCK inhibition (ROCKi) as a novel mechanism of endoderm induction in mESCs and hESCs. DE induced by the ROCK inhibitor Fasudil efficiently gives rise to PDX1+ pancreatic progenitors from hESCs. Conclusion: Taken together, DE induction by ROCKi can simplify and improve current endoderm and pancreatic differentiation protocols towards a GMP-grade cell product for β-cell replacement.

Published

2017

2. Gene Deletion Mutants Reveal a Role for Semaphorin Receptors of the Plexin-B Family in Mechanisms Underlying Corticogenesis

Author

Marcos R. Costa, Alexander Korostylev, Alexandra Hirschberg, Eszter Páldy, Stefan Offermanns, A. Wizenmann, Peter Vodrazka, Thomas Worzfeld, Rohini Kuner, Suhua Deng, and Magdalena Götz

Subjects

animal structures, SEMA4D, Neocortex, Nerve Tissue Proteins, Receptors, Cell Surface, Semaphorins, Biology, Mice, Semaphorin, Cell Movement, medicine, Animals, Receptor, Molecular Biology, Sequence Deletion, Mice, Knockout, Neurons, Genetics, Plexin, Gene Expression Regulation, Developmental, Articles, Cell Biology, Cell biology, Corticogenesis, medicine.anatomical_structure, nervous system, Mutation, embryonic structures, biology.protein, GABAergic, Ex vivo

Abstract

Semaphorins and their receptors, plexins, are emerging as key regulators of various aspects of neural and nonneural development. Semaphorin 4D (Sema4D) and B-type plexins demonstrate distinct expression patterns over critical time windows during the development of the murine neocortex. Here, analysis of mice genetically lacking plexin-B1 or plexin-B2 revealed the significance of Sema4D-plexin-B signaling in cortical development. Deficiency of plexin-B2 resulted in abnormal cortical layering and defective migration and differentiation of several subtypes of cortical neurons, including Cajal-Retzius cells, GABAergic interneurons, and principal cells in vivo. In contrast, a lack of plexin-B1 did not impact on cortical development in vivo. In various ex vivo assays on embryonic forebrain, Sema4D enhanced the radial and tangential migration of developing neurons in a plexin-B2-dependent manner. These results suggest that Sema4D-plexin-B2 interactions regulate mechanisms underlying cell specification, differentiation, and migration during corticogenesis.

Published

2010

3. The semaphorin 4D-plexin-B signalLing complex regulates dendritic and axonal complexity in developing neurons via diverse pathways

Author

Alexandra Hirschberg, Jakub M. Swiercz, Rohini Kuner, Suhua Deng, Stefan Offermanns, Alexander Korostylev, Luca Tamagnone, Thomas Worzfeld, Pietro Fazzari, and Peter Vodrazka

Subjects

animal structures, RHOA, biology, Neurite, Kinase, General Neuroscience, Plexin, SEMA4D, Receptor tyrosine kinase, Cell biology, nervous system, Semaphorin, embryonic structures, biology.protein, Growth cone, Neuroscience

Abstract

Semaphorins and their receptors, plexins, have emerged as key regulators of various aspects of neuronal development. In contrast to the Plexin-A family, the cellular functions of Plexin-B family proteins in developing neurons are only poorly understood. An activation of Plexin-B1 via its ligand, semaphorin 4D (Sema4D), produces an acute collapse of axonal growth cones in hippocampal and retinal neurons over the early stages of neurite outgrowth. However, the functional role of Sema4D-Plexin-B interactions over subsequent stages of neurite development, differentiation and maturation has not been characterized. Here we addressed this question using morphogenetic assays and time-lapse imaging on developing rat hippocampal neurons as a model system. Interestingly, Sema4D treatment over several hours was observed to promote branching and complexity in hippocampal neurons via the activation of Plexin-B1. The activation of receptor tyrosine kinases and the Rho kinase following Sema4D treatment was found to control dendritic and axonal morphogenesis by differentially regulating branching and extension. Phosphoinositide-3-kinase, but not extracellular signal-regulated kinase 1/2, was observed to be important for the stimulatory effects of Sema4D on dendritic branching. Furthermore, we observed that the mammalian target of rapamycin is activated downstream of Plexin-B1 and contributes to Sema4D-induced effects on dendritic branching. In contrast, glycogen synthase kinase-3 beta, another effector of phosphoinositide-3-kinase signalling, was not involved. Thus, our results show that Sema4D-Plexin-B interactions modulate dendritic and axonal arborizations of developing neurons by co-ordinated and concerted activation of diverse signalling pathways.

Published

2009

4. A functional role for semaphorin 4D/plexin B1 interactions in epithelial branching morphogenesis during organogenesis

Author

Jakub M. Swiercz, Roland H. Friedel, Suhua Deng, Yoshiharu Ohoka, Alexandra Hirschberg, Alexander Korostylev, Rohini Kuner, Peter Vodrazka, Viola Maier, Stefan Offermanns, Thomas Worzfeld, and Shinobu Inagaki

Subjects

animal structures, RHOA, Organogenesis, SEMA4D, Kidney development, Mice, Transgenic, Nerve Tissue Proteins, Receptors, Cell Surface, Semaphorins, Biology, Epithelium, Mesoderm, Mice, Semaphorin, Antigens, CD, Morphogenesis, Animals, RNA, Messenger, Receptor, Molecular Biology, Effector, Plexin, Immunohistochemistry, Cell biology, embryonic structures, biology.protein, Signal Transduction, Developmental Biology

Abstract

Semaphorins and their receptors, plexins, carry out important functions during development and disease. In contrast to the well-characterized plexin A family, however, very little is known about the functional relevance of B-type plexins in organogenesis, particularly outside the nervous system. Here, we demonstrate that plexin B1 and its ligand Sema4d are selectively expressed in epithelial and mesenchymal compartments during key steps in the genesis of some organs. This selective expression suggests a role in epithelial-mesenchymal interactions. Importantly, using the developing metanephros as a model system, we have observed that endogenously expressed and exogenously supplemented Sema4d inhibits branching morphogenesis during early stages of development of the ureteric collecting duct system. Our results further suggest that the RhoA-ROCK pathway, which is activated downstream of plexin B1, mediates these inhibitory morphogenetic effects of Sema4d and suppresses branch-promoting signalling effectors of the plexin B1 signalling complex. Finally, mice that lack plexin B1 show early anomalies in kidney development in vivo. These results identify a novel function for plexin B1 as a negative regulator of branching morphogenesis during kidney development, and suggest that the Sema4d-plexin B1 ligand-receptor pair contributes to epithelial-mesenchymal interactions during organogenesis via modulation of RhoA signalling.

Published

2008

5. Genetic dissection of plexin signaling in vivo

Author

Jakub M. Swiercz, Stefan Offermanns, Jingjing Xia, Jonathan A. Epstein, Thomas Worzfeld, Berit Genz, Brigitte Vollmar, Amparo Acker-Palmer, Aycan Sentürk, Rohini Kuner, Mikio Hoshino, Suhua Deng, Andrew K Chan, and Alexander Korostylev

Subjects

Multidisciplinary, RHOA, animal structures, biology, Transgene, Plexin, Mutant, Mice, Transgenic, Nerve Tissue Proteins, Biological Sciences, Phenotype, Cell biology, Mice, Semaphorin, embryonic structures, biology.protein, Animals, Guanine nucleotide exchange factor, Signal transduction, Signal Transduction

Abstract

Mammalian plexins constitute a family of transmembrane receptors for semaphorins and represent critical regulators of various processes during development of the nervous, cardiovascular, skeletal, and renal system. In vitro studies have shown that plexins exert their effects via an intracellular R-Ras/M-Ras GTPase-activating protein (GAP) domain or by activation of RhoA through interaction with Rho guanine nucleotide exchange factor proteins. However, which of these signaling pathways are relevant for plexin functions in vivo is largely unknown. Using an allelic series of transgenic mice, we show that the GAP domain of plexins constitutes their key signaling module during development. Mice in which endogenous Plexin-B2 or Plexin-D1 is replaced by transgenic versions harboring mutations in the GAP domain recapitulate the phenotypes of the respective null mutants in the developing nervous, vascular, and skeletal system. We further provide genetic evidence that, unexpectedly, the GAP domain-mediated developmental functions of plexins are not brought about via R-Ras and M-Ras inactivation. In contrast to the GAP domain mutants, Plexin-B2 transgenic mice defective in Rho guanine nucleotide exchange factor binding are viable and fertile but exhibit abnormal development of the liver vasculature. Our genetic analyses uncover the in vivo context-dependence and functional specificity of individual plexin-mediated signaling pathways during development.

Published

2014