Campbell DS , Regan AG , Lopez JS , Tannahill D , Harris WA , Holt CE .

	Fig. 1. Sema 3A induces rapid and transient collapse of retinal growth cones. A, The morphology of a retinal growth cone before the bath application of Sema 3A; B, a collapsed retinal growth cone 10 min after Sema 3A application;C, recovery of the growth cone after 60 min.D, Sema 3A induces the transient collapse of 24 hr stage 35/36 growth cones. E, Sema 3A and X-Sema 3A-induced collapse are dose dependent. *p < 0.05; Mann–Whitney U test. Scale bar (shown inA): A–C, 10 μm.
	Fig. 2. Retinal growth cones gain Sema 3A responsiveness with age. A, Sema 3A-induced collapse for 24 hr stages 24, 28, 35/36, and 37/38 retinal growth cones. Stages 35/36 and 37/38 growth cones show significant increases in collapse compared with stages 24 and 28, *p < 0.01; ANOVA.B, Sema 3A-induced collapse for 6, 24, or 48 hr stage 24 growth cones. Sema 3A-induced stage 24 growth cone collapse is significantly increased when cultured for 48 hr. *p< 0.05; Mann–Whitney U test. NP-1 and plexin expression increase in stage 24 plated retinal growth cones with duration in culture. Shown are representative photographs of NP-1 (C–E) and plexin (G–I) expression by growth cones using the A5 and B2 antibodies and a Cy3-conjugated secondary. Levels of NP-1 (F) and plexin (J) expression were quantified comparing percentage fluorescence intensity relative to control (without primary antibody). *p< 0.05; Student's t test (C,G). Sema 3A-induced collapse correlates with NP-1 expression. A 6 hr stage 24 growth cone (K) does not collapse in response to the bath application of Sema 3A (L) and does not express NP-1 (M). A 24 hr stage 35/36 growth cone (N) collapses in response to bath application of Sema 3A (O) and expresses high levels of NP-1 (P).
	Fig. 3. Precocious expression of NP-1 is sufficient to confer Sema 3A responsiveness on young retinal growth cones.A, The NP-1 antibody (AN-1) inhibits Sema 3A-induced collapse. B, A 6 hr stage 24 retinal growth cone expressing NP-1-myc. C, A collapsed growth cone expressing NP-1-myc in the presence of Sema 3A. Scale bar, 10 μm.D, Sema 3A induces the collapse of 6 hr stage 24 retinal growth cones expressing NP-1-myc. *p < 0.05; Mann–Whitney U test.
	Fig. 4. Sema 3A elicits repulsive turning in old retinal growth cones. A, A 16–26 hr stage 32 retinal growth cone before being exposed to a gradient of Sema 3A. Scale bar, 10 μm.B, After 60 min the growth cone is repelled by a gradient of Sema 3A. Traces depict the trajectories of 16–26 hr stage 32 neurites in the presence of a Sema 3A gradient applied at the black arrow (C) or X-Sema 3A gradient (D) compared with a gradient of control supernatant (Control, E).Traces depict the trajectories of 6–12 hr stage 24 retinal neurites in the presence of a gradient of Sema 3A that does not induce repulsive turning (F) and control (G). H, Cumulative frequency graph showing the distribution of turning angles for stages 32 and 24 retinal growth cones, Sema 3A, and control. Sema 3A and X-Sema 3A are repulsive to growth cones from stage 32 plated retinal explants; i.e., most of the turning angles are negative relative to control turning angles and the turning angles for a gradient of Sema 3A on stage 24 growth cones and control. I, Mean turning, Sema 3A, and X-Sema 3A induce significant repulsion of stage 32 retinal growth cones. *p < 0.05; Kolmogorov–Smirnov test.
	Fig. 5. Sema 3A elicits branching after recovery from collapse. A, A 24 hr stage 35/36 retinal growth cone before the application of Sema 3A. B, The same growth exhibiting collapsed morphology after 10 min. C, After 30 min the growth cone has begun to branch. D, After 60 min the branch remains. Scale bar, 10 μm. E, Sema 3A induces the branching of retinal growth cones. Cumulative branching in the most distal 100 μm of neurite growth illustrates that the majority of the branching occurs within approximately the first 35 μm, the mean neurite growth in 1 hr. *p < 0.05; Mann–Whitney U test.
	Fig. 6. Pharmacological perturbation of cGMP signaling modulates the responses to Sema 3A. Pharmacological perturbation of cGMP signaling but not cAMP signaling via the activation or inhibition of protein kinase G significantly reduces 24 hr stage 35/36 Sema 3A-induced growth cone collapse (A). *p < 0.05; Mann–Whitney U test.Traces depict the trajectories of 16–26 hr stage 32 retinal neurites in the presence of pharmacological modulators of cGMP and cAMP signaling (B–E) in the medium and a directional source of Sema 3A. B, The activation of PKG with 100 μm 8-BrcGMP converts Sema 3A-induced repulsion to attraction. p < 0.01; Kolmogorov–Smirnov test.C, Inhibition of PKG with 10 μm RpcGMPS abolishes Sema 3A-induced repulsion, leading to a heterogeneous turning response. D, E, Activation or inhibition of PKA with 20 μm SpcAMPS or RpAMPS does not significantly affect Sema 3A-induced repulsion. F, Cumulative frequency graph showing the turning angles to Sema 3A. In the presence of 100 μm 8-BrcGMP, the curve is shifted to theright. With 10 μm RpcGMPS, approximately equal numbers of angles lie on either side, and with 20 μm SpcAMPS or RpcAMPS, most turning angles lie to theleft, indicating repulsion. G, Activation or inhibition of PKG inhibits Sema 3A-induced branching. *p < 0.05; Mann–Whitney Utest.
	Fig. 7. Sema 3A expression in the developing optic pathway. Shown are whole-mount lateral views of stage 33/34 (A) and stage 41 (B–D) Xenopus brains in which the RGCs have been anterogradely filled with HRP and visualized with DAB. Sema 3A is highly expressed in the telencephalon, hindbrain, and posterior tectum but not in the optic tract (A,B). Shown is magnified view of Sema 3A expression in the diencephalon (C) and posterior tectum (D) illustrating its proximity to the RGC axons. Shown are horizontal paraffin sections at the level of the tectum (E) and telencephalon (F). The level of the sections in E and F is denoted by the white arrow in B, labeleda and b, respectively. Di, Diencephalon; Hb, hindbrain; Hy, hypothalamus; Ot, optic tract; Tec, tectum; Tel, telencephalon. White arrowheads indicate the midbrain/hindbrain boundary.Black arrowheads highlight the HRP-filled RGC axons. Scale bar (shown in A): A,B, E, F, 100 μm;C, D, 50 μm. Anterior is to theright.

Acebes, Cellular and molecular features of axon collaterals and dendrites. 2000, Pubmed

Acebes, Cellular and molecular features of axon collaterals and dendrites. 2000, Pubmed
Bagnard, Semaphorins act as attractive and repulsive guidance signals during the development of cortical projections. 1998, Pubmed
Brose, Slit proteins: key regulators of axon guidance, axonal branching, and cell migration. 2000, Pubmed
Castellani, Dual action of a ligand for Eph receptor tyrosine kinases on specific populations of axons during the development of cortical circuits. 1998, Pubmed
Chien, Axonal guidance from retina to tectum in embryonic Xenopus. 1994, Pubmed , Xenbase
Cohen-Cory, Effects of brain-derived neurotrophic factor on optic axon branching and remodelling in vivo. 1995, Pubmed , Xenbase
Cornel, Precocious pathfinding: retinal axons can navigate in an axonless brain. 1992, Pubmed , Xenbase
Davenport, Neuronal growth cone collapse triggers lateral extensions along trailing axons. 1999, Pubmed
Dingwell, The multiple decisions made by growth cones of RGCs as they navigate from the retina to the tectum in Xenopus embryos. 2000, Pubmed , Xenbase
Fan, Localized collapsing cues can steer growth cones without inducing their full collapse. 1995, Pubmed
Fujisawa, Growth-associated expression of a membrane protein, neuropilin, in Xenopus optic nerve fibers. 1995, Pubmed , Xenbase
Halloran, Analysis of a Zebrafish semaphorin reveals potential functions in vivo. 1999, Pubmed
Harris, Retinal axons with and without their somata, growing to and arborizing in the tectum of Xenopus embryos: a time-lapse video study of single fibres in vivo. 1987, Pubmed , Xenbase
He, Neuropilin is a receptor for the axonal chemorepellent Semaphorin III. 1997, Pubmed
Heffner, Target control of collateral extension and directional axon growth in the mammalian brain. 1990, Pubmed
Hemmati-Brivanlou, Cephalic expression and molecular characterization of Xenopus En-2. 1991, Pubmed , Xenbase
Holt, Does timing of axon outgrowth influence initial retinotectal topography in Xenopus? 1984, Pubmed , Xenbase
Höpker, Growth-cone attraction to netrin-1 is converted to repulsion by laminin-1. 1999, Pubmed , Xenbase
Kalil, Common mechanisms underlying growth cone guidance and axon branching. 2000, Pubmed
Kameyama, Identification of a neuronal cell surface molecule, plexin, in mice. 1996, Pubmed , Xenbase
Kawakami, Developmentally regulated expression of a cell surface protein, neuropilin, in the mouse nervous system. 1996, Pubmed , Xenbase
Kolodkin, Growth cones and the cues that repel them. 1996, Pubmed
Kolodkin, Neuropilin is a semaphorin III receptor. 1997, Pubmed
Lohof, Asymmetric modulation of cytosolic cAMP activity induces growth cone turning. 1992, Pubmed , Xenbase
Luo, Collapsin: a protein in brain that induces the collapse and paralysis of neuronal growth cones. 1993, Pubmed
Luo, A family of molecules related to collapsin in the embryonic chick nervous system. 1995, Pubmed
Messersmith, Semaphorin III can function as a selective chemorepellent to pattern sensory projections in the spinal cord. 1995, Pubmed
Ming, cAMP-dependent growth cone guidance by netrin-1. 1997, Pubmed , Xenbase
Murakami, Differential expression of plexin-A subfamily members in the mouse nervous system. 2001, Pubmed
Niwa, Efficient selection for high-expression transfectants with a novel eukaryotic vector. 1991, Pubmed
Ohta, Involvement of neuronal cell surface molecule B2 in the formation of retinal plexiform layers. 1992, Pubmed , Xenbase
Ohta, Plexin: a novel neuronal cell surface molecule that mediates cell adhesion via a homophilic binding mechanism in the presence of calcium ions. 1995, Pubmed , Xenbase
Ohta, Embryonic lens repels retinal ganglion cell axons. 1999, Pubmed
Pasterkamp, Evidence for a role of the chemorepellent semaphorin III and its receptor neuropilin-1 in the regeneration of primary olfactory axons. 1998, Pubmed
Polleux, Semaphorin 3A is a chemoattractant for cortical apical dendrites. 2000, Pubmed
Püschel, Murine semaphorin D/collapsin is a member of a diverse gene family and creates domains inhibitory for axonal extension. 1995, Pubmed
Raper, The enrichment of a neuronal growth cone collapsing activity from embryonic chick brain. 1990, Pubmed
Renzi, Olfactory sensory axons expressing a dominant-negative semaphorin receptor enter the CNS early and overshoot their target. 2000, Pubmed
Rohm, Plexin/neuropilin complexes mediate repulsion by the axonal guidance signal semaphorin 3A. 2000, Pubmed
Shimamura, Wnt-1-dependent regulation of local E-cadherin and alpha N-catenin expression in the embryonic mouse brain. 1994, Pubmed
Shirasaki, Change in chemoattractant responsiveness of developing axons at an intermediate target. 1998, Pubmed
Shoji, Zebrafish semaphorin Z1a collapses specific growth cones and alters their pathway in vivo. 1998, Pubmed
Song, Conversion of neuronal growth cone responses from repulsion to attraction by cyclic nucleotides. 1998, Pubmed , Xenbase
Straznicky, The development of the tectum in Xenopus laevis: an autoradiographic study. 1972, Pubmed , Xenbase
Takagi, The A5 antigen, a candidate for the neuronal recognition molecule, has homologies to complement components and coagulation factors. 1991, Pubmed , Xenbase
Takagi, Specific cell surface labels in the visual centers of Xenopus laevis tadpole identified using monoclonal antibodies. 1987, Pubmed , Xenbase
Takagi, Expression of a cell adhesion molecule, neuropilin, in the developing chick nervous system. 1995, Pubmed , Xenbase
Takahashi, Plexin-neuropilin-1 complexes form functional semaphorin-3A receptors. 1999, Pubmed
Takahashi, Semaphorins A and E act as antagonists of neuropilin-1 and agonists of neuropilin-2 receptors. 1998, Pubmed
Tamagnone, Plexins are a large family of receptors for transmembrane, secreted, and GPI-anchored semaphorins in vertebrates. 1999, Pubmed , Xenbase
Taniguchi, Disruption of semaphorin III/D gene causes severe abnormality in peripheral nerve projection. 1997, Pubmed
Tessier-Lavigne, The molecular biology of axon guidance. 1996, Pubmed
Tuttle, Neurotrophins rapidly modulate growth cone response to the axon guidance molecule, collapsin-1. 1998, Pubmed
Varela-Echavarría, Motor axon subpopulations respond differentially to the chemorepellents netrin-1 and semaphorin D. 1997, Pubmed
Wang, Biochemical purification of a mammalian slit protein as a positive regulator of sensory axon elongation and branching. 1999, Pubmed
Weeks, cAMP promotes branching of laminin-induced neuronal processes. 1991, Pubmed
Yee, Molecular cloning, expression, and activity of zebrafish semaphorin Z1a. 1999, Pubmed
Zheng, Turning of nerve growth cones induced by neurotransmitters. 1994, Pubmed , Xenbase
Zou, Squeezing axons out of the gray matter: a role for slit and semaphorin proteins from midline and ventral spinal cord. 2000, Pubmed
de la Torre, Turning of retinal growth cones in a netrin-1 gradient mediated by the netrin receptor DCC. 1997, Pubmed , Xenbase