Microtubule organization in growth cones.
نویسنده
چکیده
13. Albelda. S. M. & Huck. C. A. (1990) FASEH J. 4, 2868-2880 Kouslahti, E. (1001) J. Clin. Invest. 87. 1-’5 Hurridge. K., Fath, K., Kelly, T., Nuckolis, H. & Turner. C. (1988) Annu. Rev. Cell Hiol. 4, 487-525 Tamkun, J. W.. l)eSimone, I). W.. Fonda, I).? I’atel, K. S., Huck, C. A., Horwitz, A. F. & Hynes, K. 0. (1986) Cell (Cambridge. Mass.) 46,271-282 Springer, T. A. (1990) Nature (London) 346, 425-434 Ekes, M. J., Osborn, I,.. Takada, Y.. Crouse, C., lahowsky, S., [Iemler. M. E. & I,obb, K. K. (1090) Cell (Cambridge. Mass.) 60. 577-584 Kemler. K.. Ozaua. M. & Kingwald, M. (1080) Curr. Opinion Cell Hiol. 1, 802-807 Takeichi, M. (1001) Science 251. 3451-1455 Ozawa. M., Haribault, 11. & Keniler, K. (1080) EMHO J. 8. 171 1-1717 Williams, A. I;. & 13arcIay. A. N. (1088) Annu. Kev.. Immunol. 6, 38 1-405 Hurgoon, M. l’.. Grumet, M., Mauro,’V.. Edelman, G. M. & Cunningham, H. A. (1901) J. Cell I3iol. 112, 10 171029 14. Henchimol. S.. Fuks. A., Jothy, S., Heauchemin. N.. Shirota, K. & Stanners, C. 1’. (1980) Cell (Cambridge, Mass.) 57, 327-334 15. Springer, T. A. & Lasky, 1,. A. (1901) Nature (London) 349. 106-107 16. Feizi, T. (1991) Trends Hiochem. Sci. 16, 84-86 17. Fehon, K. G., Kooh, P. J., Kebay, I., Kegan, C. L., Xu, T., Muskavitch, M. A. T. & Artavanis-Tsakonas, S. (1990) Cell (Cambridge, Mass.) 61. 523-534 18. Tepass, U.. Theres, C. & Knust, E. (1990) Cell (Cambridge, Mass.) 61, 787-799 10. Fehon, K. G., Johansen, K., Kebay, 1. & ArtavanisTsakonas. S. (1001) J. Cell Hiol. 113, 057-660 20 Furie, 13. & Furic. H. C (1088) Cell (Cambridge, Mass ) 53,505-5 I 8 21 Stoolman, I,. M (1080) Cell (Cambridge, Mass.) 56. 007-010 22. Gloor, S., Antonicek, H.. Sweadner, K. I,., I’agliusi, S., Frank. K., Moos, M. & Schachner, M. (1090) J. Cell Hiol. 110, 165-175
منابع مشابه
Microtubule reorganization is obligatory for growth cone turning.
To examine the role of microtubules in growth cone turning, we have compared the microtubule organization in growth cones advancing on uniform laminin substrates with their organization in growth cones turning at a laminin-tenascin border. The majority (82%) of growth cones on laminin had a symmetrical microtubule organization, in which the microtubules entering the growth cone splay out toward...
متن کاملEvidence for the role of MAP1B in axon formation.
Cultured neurons obtained from a hypomorphous MAP1B mutant mouse line display a selective and significant inhibition of axon formation that reflects a delay in axon outgrowth and a reduced rate of elongation. This phenomenon is paralleled by decreased microtubule formation and dynamics, which is dramatic at the distal axonal segment, as well as in growth cones, where the more recently assembled...
متن کاملThe kinesin-2 family member KIF3C regulates microtubule dynamics and is required for axon growth and regeneration.
Axon regeneration after injury requires the extensive reconstruction, reorganization, and stabilization of the microtubule cytoskeleton in the growth cones. Here, we identify KIF3C as a key regulator of axonal growth and regeneration by controlling microtubule dynamics and organization in the growth cone. KIF3C is developmentally regulated. Rat embryonic sensory axons and growth cones contain u...
متن کاملCNP/cGMP signaling regulates axon branching and growth by modulating microtubule polymerization.
The peptide hormone CNP has recently been found to positively regulate axon branching and growth via activation of cGMP signaling in embryonic dorsal root ganglion (DRG) neurons, but the cellular mechanisms mediating the regulation of these developmental processes have not been established. In this study, we provide evidence linking CNP/cGMP signaling to microtubule dynamics via the microtubule...
متن کاملThe Ubiquitin Ligase Phr1 Regulates Axon Outgrowth through Modulation of Microtubule Dynamics
To discover new genes involved in axon navigation, we conducted a forward genetic screen for recessive alleles affecting motor neuron pathfinding in GFP reporter mice mutagenized with ENU. In Magellan mutant embryos, motor axons were error prone and wandered inefficiently at choice points within embryos, but paradoxically responded to guidance cues with normal sensitivity in vitro. We mapped th...
متن کاملDisorganized microtubules underlie the formation of retraction bulbs and the failure of axonal regeneration.
Axons in the CNS do not regrow after injury, whereas lesioned axons in the peripheral nervous system (PNS) regenerate. Lesioned CNS axons form characteristic swellings at their tips known as retraction bulbs, which are the nongrowing counterparts of growth cones. Although much progress has been made in identifying intracellular and molecular mechanisms that regulate growth cone locomotion and a...
متن کاملذخیره در منابع من
با ذخیره ی این منبع در منابع من، دسترسی به آن را برای استفاده های بعدی آسان تر کنید
برای دانلود متن کامل این مقاله و بیش از 32 میلیون مقاله دیگر ابتدا ثبت نام کنید
ثبت ناماگر عضو سایت هستید لطفا وارد حساب کاربری خود شوید
ورودعنوان ژورنال:
- Biochemical Society transactions
دوره 19 4 شماره
صفحات -
تاریخ انتشار 1991