संवर्धित वयस्क पृष्ठीय रूट नाड़ीग्रन्थि न्यूरॉन्स साथ Axon पुनर्जनन की आनुवंशिक अध्ययन
Summary
एक<em> इन विट्रो में</em> अक्षतंतु उत्थान का उपयोग सुसंस्कृत वयस्क माउस पृष्ठीय रूट नाड़ीग्रन्थि न्यूरॉन्स की आनुवंशिक अध्ययन के लिए मॉडल में वर्णित है. इस विधि आनुवंशिक हेरफेर के दौर से गुजर न्यूरॉन्स से कदम अक्षतंतु फिर से विकास की अनुमति re-suspension/re-plating शामिल हैं. इस दृष्टिकोण अक्षतंतु उत्थान के नुकसान के समारोह के अध्ययन आरएनएआई आधारित प्रोटीन पछाड़ना का उपयोग करने के लिए विशेष रूप से उपयोगी है.
Abstract
It is well known that mature neurons in the central nervous system (CNS) cannot regenerate their axons after injuries due to diminished intrinsic ability to support axon growth and a hostile environment in the mature CNS1,2. In contrast, mature neurons in the peripheral nervous system (PNS) regenerate readily after injuries3. Adult dorsal root ganglion (DRG) neurons are well known to regenerate robustly after peripheral nerve injuries. Each DRG neuron grows one axon from the cell soma, which branches into two axonal branches: a peripheral branch innervating peripheral targets and a central branch extending into the spinal cord. Injury of the DRG peripheral axons results in substantial axon regeneration, whereas central axons in the spinal cord regenerate poorly after the injury. However, if the peripheral axonal injury occurs prior to the spinal cord injury (a process called the conditioning lesion), regeneration of central axons is greatly improved4. Moreover, the central axons of DRG neurons share the same hostile environment as descending corticospinal axons in the spinal cord. Together, it is hypothesized that the molecular mechanisms controlling axon regeneration of adult DRG neurons can be harnessed to enhance CNS axon regeneration. As a result, adult DRG neurons are now widely used as a model system to study regenerative axon growth5-7.
Here we describe a method of adult DRG neuron culture that can be used for genetic study of axon regeneration in vitro. In this model adult DRG neurons are genetically manipulated via electroporation-mediated gene transfection6,8. By transfecting neurons with DNA plasmid or si/shRNA, this approach enables both gain- and loss-of-function experiments to investigate the role of any gene-of-interest in axon growth from adult DRG neurons. When neurons are transfected with si/shRNA, the targeted endogenous protein is usually depleted after 3-4 days in culture, during which time robust axon growth has already occurred, making the loss-of-function studies less effective. To solve this problem, the method described here includes a re-suspension and re-plating step after transfection, which allows axons to re-grow from neurons in the absence of the targeted protein. Finally, we provide an example of using this in vitro model to study the role of an axon regeneration-associated gene, c-Jun, in mediating axon growth from adult DRG neurons9.
Protocol
Discussion
वयस्क DRG न्यूरॉन्स और vivo में इन विट्रो में परिधीय तंत्रिका चोट के बाद मजबूती के साथ उनके axons पुनर्जन्म, इस प्रकार अक्षतंतु उत्थान के लिए वयस्क पशुओं में अध्ययन के लिए एक उपयोगी प्रणाली प्रदान करते हैं….
Declarações
The authors have nothing to disclose.
Acknowledgements
इस काम FZ करने के लिए (R01NS064288) NIH और क्रेग एच. Neilsen फाउंडेशन से अनुदान द्वारा समर्थित किया गया.
Materials
| Name of the reagent | Company | Catalogue number |
| MEM | Invitrogen | 11090-081 |
| Poly-D-Lysine hydrobromide | Sigma -Aldrich | P6407 |
| Laminin | Invitrogen | 23017-015 |
| 5-fluoro-2-deoxyuridine | Sigma -Aldrich | F0503 |
| Uridine | Sigma -Aldrich | U3003 |
| Collagenase A | Roche | 10103578001 |
| TrypLE Express | Invitrogen | 12604-013 |
| Fetal bovine serum | Invitrogen | 10270-098 |
| Penicillin-streptomycin (100X) | Invitrogen | 15140-122 |
| GlutaMAX-I (100X) | Invitrogen | 35050-038 |
| Glass coverslips (#1) | Electron Microscopy sciences | 72196-12 |
| 24 well cell culture plate | Becton Dickinson | 35-3047 |
| 1X PBS | Mediatech | 21-040-CV |
| Sterile, distilled and deionized water | Mediatech | 25-055-CV |
| Nucleofector and electroporation Kits for Mouse Neurons | Lonza | VPG-1001 |
| ON-TARGETplus siRNA against c-Jun | Dharmacon | L-043776 |
| Anti–βIII tubulin antibody (Tuj-1) | Covance | MMS-435P |
| ProLong Gold Antifade mounting solution | Invitrogen | P36930 |
Referências
- Yiu, G., He, Z. Glial inhibition of CNS axon regeneration. Nat. Rev. Neurosci. 7, 617-627 (2006).
- Liu, K., Tedeschi, A., Park, K. K., He, Z. Neuronal Intrinsic Mechanisms of Axon Regeneration. Annu. Rev. Neurosci. , (2010).
- Zhou, F. Q., Snider, W. D. Intracellular control of developmental and regenerative axon growth. Philos. Trans. R. Soc. Lond. B. Biol. Sci. 361, 1575-1592 (2006).
- Neumann, S., Woolf, C. J. Regeneration of dorsal column fibers into and beyond the lesion site following adult spinal cord injury. Neuron. 23, 83-91 (1999).
- Liu, R. Y., Snider, W. D. Different signaling pathways mediate regenerative versus developmental sensory axon growth. J. Neurosci. 21, RC164 (2001).
- Zhou, F. Q. Neurotrophins support regenerative axon assembly over CSPGs by an ECM-integrin-independent mechanism. J. Cell Sci. 119, 2787-2796 (2006).
- Zou, H., Ho, C., Wong, K., Tessier-Lavigne, M. Axotomy-induced Smad1 activation promotes axonal growth in adult sensory neurons. J. Neurosci. 29, 7116-7123 (2009).
- Zhou, F. Q., Zhou, J., Dedhar, S., Wu, Y. H., Snider, W. D. NGF-induced axon growth is mediated by localized inactivation of GSK-3beta and functions of the microtubule plus end binding protein APC. Neuron. 42, 897-912 (2004).
- Saijilafu, E. M., Hur, F. Q., Zhou, Genetic dissection of axon regeneration via in vivo electroporation of adult mouse sensory neurons. Nat. Commun. 2, 543-54 (2011).
- Costigan, M. Replicate high-density rat genome oligonucleotide microarrays reveal hundreds of regulated genes in the dorsal root ganglion after peripheral nerve injury. BMC Neurosci. 3, 16 (2002).
- Xiao, H. S. Identification of gene expression profile of dorsal root ganglion in the rat peripheral axotomy model of neuropathic pain. Proc. Natl. Acad. Sci. U.S.A. 99, 8360-8365 (2002).
- Michaelevski, I. Signaling to transcription networks in the neuronal retrograde injury response. Sci. Signal. 3, ra53 (2010).
