Summary

العصب الشظية الإصابات الطريقة: مقايسة موثوقة لتحديد واختبار العوامل التي إصلاح العضلية المفارق

Published: August 11, 2016
doi:

Summary

We have developed a nerve injury method to reliably examine muscle reinnervation, and thus regeneration of neuromuscular junctions in mice. This technique involves injuring the common fibular nerve via a simple and highly reproducible surgery. Muscle reinnervation in then assessed by whole-mounting the extensor digitorum longus muscle.

Abstract

الوصل العصبي العضلي (NMJ) يخضع لتغيرات هيكلية ووظيفية الضارة نتيجة للتقدم في السن والإصابات والأمراض. وبالتالي، لا بد من فهم التغيرات الخلوية والجزيئية تشارك في صيانة وإصلاح لل NMJs. لهذا الغرض، قمنا بتطوير طريقة وبشكل متواصل لدراسة تجديد لل NMJs في الفئران. هذه الطريقة إصابة العصب ينطوي على سحق العصب الشظوي المشترك لأنه يمر فوق الرأس الوحشي من وتر عضلة الساق بالقرب من الركبة. استخدام 70 يوم إناث الفئران القديمة، علينا أن نبرهن على المحاور الحركية تبدأ reinnervate الأهداف بعد المشبكي السابقة خلال 7 أيام بعد سحق. انهم إعادة احتلال المناطق تماما متشابك السابقة من قبل 12 يوما. لتحديد موثوقية هذه الطريقة الإصابة، قارنا معدلات عودة التعصيب بين الأفراد 70 يوم إناث الفئران القديمة. وجدنا أن عدد المواقع بعد المشبكي reinnervated مماثل بين الفئران في 7 و 9 و 12 يوما بعد سحق. لتحديد ما إذا كانويمكن أيضا أن هذا الاختبار إصابة استخدامها لمقارنة التغيرات الجزيئية في العضلات، درسنا مستويات غاما فرعية من مستقبلات العضلات النيكوتينيك (غاما الاستشاري لحقوق الإنسان) وكيناز العضلات محددة (المسك). الوحيدات غاما الاستشاري لحقوق الإنسان والمسك لوupregulated للغاية إزالة التعصيب التالية والعودة إلى مستويات طبيعية بعد عودة التعصيب من لل NMJs. لقد وجدنا علاقة وثيقة بين مستويات النص لهذه الجينات ووضع تعصيب العضلات. ونحن نعتقد أن هذا الأسلوب سيعجل فهمنا للتغيرات الخلوية والجزيئية تشارك في إصلاح NMJ ونقاط الاشتباك العصبي الأخرى.

Introduction

In young adult and healthy animals, the neuromuscular junction (NMJ) is a highly stable connection between the presynapse, the nerve ending of an α-motor axon, and the postsynapse, the specialized region of an extrafusal muscle fiber where nicotinic acetylcholine receptors (AChRs) selectively aggregate1. The nearly perfect apposition of the pre- and post-synaptic apparatuses is necessary for proper neurotransmission, survival of α-motor neurons and muscle fibers and motor function. Unfortunately, the function of the NMJ is adversely affected by aging, diseases such as amyotrophic lateral sclerosis (ALS), autoimmune diseases and injury to muscles and peripheral nerves2-5. These insults often result in degeneration of presynaptic nerve endings, leaving muscles denervated and significantly altering motor skills. For this reason, the identification of molecules that function to maintain and repair the NMJ has become a priority. Because peripheral nerves regenerate and reinnervate targets, peripheral nerve injury models have been used to identify molecular changes associated with regenerating NMJs.

Peripheral nerve injury models often involve either completely cutting or crushing specific nerve branches6. Following a cut, the endoneurial tube has to be reformed, delaying axonal regeneration and reinnervation of target cells and tissues. The severity of this type of injury also causes axons to meander away from their original path, resulting in their failure to reach original targets. This is in contrast to nerves injured via crush where the endoneurium remains contiguous, providing a path for efficient and proper regrowth of regenerating axons. It also allows axons to find and reinnervate their original muscle fiber partners. Irrespective of injury model, there are a number of cellular and molecular changes that must occur for axons to regenerate and reinnervate targets. After an injury, the nerve segment proximal to the target is broken down and removed via a process termed Wallerian Degeneration7. This process involves reprogramming and de-differentiation of Schwann cells into non-myelinating cells that secrete regenerative factors, clear myelin, and recruit macrophages to the site of injury8. Macrophages in turn complete the clearance of myelin and axonal debris, which would otherwise impede growth of the regenerating axon9. In parallel, motor and sensory neurons activate mechanisms needed to promote regeneration of their severed axons. Once the regenerating axon reaches the target, it must transform from a growth cone to a nerve ending capable of properly transmitting (for motor axons) or receiving (for sensory axons) information10. In this regard, alpha-motor axons undergo a series of well-orchestrated changes that culminate in their growth cone differentiating into a fully functional presynaptic nerve ending that nearly perfectly opposes the post-synaptic site on the target muscle fiber11.

The sciatic, tibial and accessory nerves have been the primary choices for studying axonal and NMJ regeneration12-14. However, there are a number of drawbacks when using these models to examine cellular and molecular changes associated with regenerating NMJs between animals and under different conditions. Firstly, the sciatic nerve supplies the majority of the muscles of the hind limb, with injury significantly limiting both movement and sensation. It is therefore not possible to use this method to study the impact of exercise alone or in combination with other factors. Additionally, the sciatic nerve is a rather thick structure and thus requires a large amount of compressive force to fully injure all axons. This in turn may result in complete transection of the more superficial axons while leaving the endoneurial tube of deeper lying axons intact, introducing significant variability in the rate and fidelity of regeneration among these axons. Complete transection of this nerve is even less desirable given that many axons will fail to reconnect with the same muscle fibers. Complicating matters, the sciatic nerve possesses intrinsic anatomic variability, both in the number and site of origin of its terminal nerve branches. It is therefore very difficult to lesion the same site. While the tibial nerve is smaller and more amenable to crush injuries, there is also no readily available landmark to serve as a lesion site for this nerve branch.

The accessory nerve branch (part of cranial nerve XI) that supplies the sternocleidomastoid muscle has also been used to study regeneration of NMJs15. This nerve is particularly attractive because NMJs in the sternocleidomastoid muscle can be more readily imaged in live animals compared to NMJs in other muscles. But similar to the sciatic and tibial nerves, there is no specific landmark that can be used to injure this nerve in the same location, limiting it as a model for comparing regeneration of NMJs among individual animals of an experimental cohort. An inconsistent lesion site introduces variability in the rates of NMJ reinnervation. Due to these shortcomings, the procedure presented here utilizes the injury of a different peripheral nerve branch to examine regenerating NMJs.

The common fibular nerve, also called the common peroneal nerve, contains many features that make it a reliable nerve to examine regeneration of NMJs between animals and across different treatments. The common fibular nerve has a predictable anatomic course as it runs over the tendon of the lateral head of the gastrocnemius muscle in the knee, the intersection serving as a stable landmark for lesions. The nerve is accessed through a small and minimally invasive incision near but anatomically segregated from the muscles of interest. The findings presented here demonstrate that regenerating motor axons begin to reform NMJs in the extensor digitorum longus (EDL) muscle 8 days after crushing the fibular nerve in 70 days old young adult female mice. Importantly, the pattern and rate of reinnervation is consistent among animals of the same age and sex and therefore provide a reliable injury model that will significantly hasten our understanding of the cellular and molecular changes required to maintain and repair NMJs.

Protocol

أجريت جميع التجارب تحت المبادئ التوجيهية المعاهد الوطنية للصحة والبروتوكولات الحيوانية التي وافقت عليها لجنة جامعة فرجينيا للتكنولوجيا المؤسسي رعاية الحيوان واستخدام. 1. الحيوانات التحضير لجراحة <li style…

Representative Results

العصب الشظوي المشترك، وتسمى أيضا العصب الشظوي المشترك، ينشأ من العصب الوركي فوق المبأبضية، حيث يتأرجح حول رأس الشظية على الجانب الأمامي للساق (الشكل 1A). هناك فروع لها في الأعصاب الشظوية سطحية وعميقة، جنبا إلى جنب تزويد dorsiflexors القدم وأصابع …

Discussion

الطريقة المعروضة في هذه المخطوطة يوفر فرصا فريدة لتحديد الآليات التي تشارك في إصلاح الوصلات العصبية والعضلية (NMJ). هذا الأسلوب ينطوي على سحق العصب الشظوي المشترك لأنها تمر على وتر الساق بالقرب من الركبة. وتبين لنا أنه بعد ثانية فقط 5 من ضغط العصب مع ملقط، يلاحظ انحطاط ?…

Offenlegungen

The authors have nothing to disclose.

Acknowledgements

The authors thank members of the Valdez laboratory for intellectual input on experiments and comments on the manuscript.

Materials

Ketamine VetOne  501072 
Xylazine Lloyd Inc.  003437 
Buprenorphine  Zoopharm 1Z-73000-150910 
Nair Nair
Kim-wipes Kimtech 34155
Electric Razor Braintree Scientific CLP-64800
80% EtOH/H20
10% Proviodine
1 mL Insulin Syringe
Spring Scissors Vannas 91500-09
No. 15 scalpel Braintree Scientific SSS 15
#5 Forceps Dumont 11252-00
6-0 silk suture on reverse cutting needle  Suture Express 752B 
Rodent Heating Pad Braintree Scientific AP-R-18.5
Alexa 555 conjugated alpha-BTX Molecular Probes B35451
Vectashield Vector Labs H-1000
Olympus Stereo Zoom Microscope Olympus 562037192
Zeiss 700 Confocal Microscope Zeiss
Variable-flow peristaltic perfusion pump Fisher Scientific 13-876-3
Aurum Total RNA Mini Kit Bio-Rad 7326820
Bio-Rad iScript RT Supermix Bio-Rad 1708840
SsoFast Evagreen Supermix Bio-Rad 1725200
Bio-Rad CFX96 Bio-Rad 1855196
Puralube vet ointment Puralube 1621
Synaptotagmin-2 antibody Antibodies-Online ABIN401605
Neurofilament antibody Antibodies-Online ABIN2475842

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Dalkin, W., Taetzsch, T., Valdez, G. The Fibular Nerve Injury Method: A Reliable Assay to Identify and Test Factors That Repair Neuromuscular Junctions. J. Vis. Exp. (114), e54186, doi:10.3791/54186 (2016).

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