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Literature DB >> 34717939

IL-4 expressing cells are recruited to nerve after injury and promote regeneration.

Deng Pan¹, Lauren Schellhardt¹, Jesús A Acevedo-Cintron¹, Daniel Hunter¹, Alison K Snyder-Warwick¹, Susan E Mackinnon¹, Matthew D Wood².

Abstract

Interleukin-4 (IL-4) has garnered interest as a cytokine that mediates regeneration across multiple tissues including peripheral nerve. Within nerve, we previously showed endogenous IL-4 was critical to regeneration across nerve gaps. Here, we determined a generalizable role of IL-4 in nerve injury and regeneration. In wild-type (WT) mice receiving a sciatic nerve crush, IL-4 expressing cells preferentially accumulated within the injured nerve compared to affected sites proximal, such as dorsal root ganglia (DRGs), or distal muscle. Immunohistochemistry and flow cytometry confirmed that eosinophils (CD45+, CD11b+, CD64-, Siglec-F+) were sources of IL-4 expression. Examination of targets for IL-4 within nerve revealed macrophages, as well as subsets of neurons expressed IL-4R, while Schwann cells expressed limited IL-4R. Dorsal root ganglia cultures were exposed to IL-4 and demonstrated an increased proportion of neurons that extended axons compared to cultures without IL-4 (control), as well as longer myelinated axons compared to cultures without IL-4. The role of endogenous IL-4 during nerve injury and regeneration in vivo was assessed following a sciatic nerve crush using IL-4 knockout (KO) mice. Loss of IL-4 affected macrophage accumulation within injured nerve compared to WT mice, as well as shifted macrophage phenotype towards a CD206- phenotype with altered gene expression. Furthermore, this loss of IL-4 delayed initial axon regeneration from the injury crush site and subsequently delayed functional recovery and re-innervation of neuromuscular junctions compared to wild-type mice. Given the role of endogenous IL-4 in nerve regeneration, exogenous IL-4 was administered daily to WT mice following a nerve crush to examine regeneration. Daily IL-4 administration increased early axonal extension and CD206+ macrophage accumulation but did not alter functional recovery compared to untreated mice. Our data demonstrate IL-4 promotes nerve regeneration and recovery after injury.

Entities: Chemical

Keywords: Functional recovery; IL-4; Interleukin; Macrophage; Nerve crush; Nerve regeneration; Peripheral nerve

Mesh：

Substances：

Year: 2021 PMID： 34717939 PMCID： PMC8887027 DOI： 10.1016/j.expneurol.2021.113909

Source DB: PubMed Journal: Exp Neurol ISSN： 0014-4886 Impact factor: 5.330

31 in total

1. IL-4 acts as a myoblast recruitment factor during mammalian muscle growth.

Authors: Valerie Horsley; Katie M Jansen; Stephen T Mills; Grace K Pavlath
Journal: Cell Date: 2003-05-16 Impact factor: 41.582

2. Macrophages Regulate Schwann Cell Maturation after Nerve Injury.

Authors: Jo Anne Stratton; Alexandra Holmes; Nicole L Rosin; Sarthak Sinha; Mohit Vohra; Nicole E Burma; Tuan Trang; Rajiv Midha; Jeff Biernaskie
Journal: Cell Rep Date: 2018-09-04 Impact factor: 9.423

Review 3. The multicellular complexity of peripheral nerve regeneration.

Authors: Anne-Laure Cattin; Alison C Lloyd
Journal: Curr Opin Neurobiol Date: 2016-04-26 Impact factor: 6.627

4. The CCL2/CCR2 axis is critical to recruiting macrophages into acellular nerve allograft bridging a nerve gap to promote angiogenesis and regeneration.

Authors: Deng Pan; Jesús A Acevedo-Cintrón; Junichi Sayanagi; Alison K Snyder-Warwick; Susan E Mackinnon; Matthew D Wood
Journal: Exp Neurol Date: 2020-05-23 Impact factor: 5.330

5. Fast direct neuronal signaling via the IL-4 receptor as therapeutic target in neuroinflammation.

Authors: Christina F Vogelaar; Shibajee Mandal; Steffen Lerch; Katharina Birkner; Jerome Birkenstock; Ulrike Bühler; Andrea Schnatz; Cedric S Raine; Stefan Bittner; Johannes Vogt; Jonathan Kipnis; Robert Nitsch; Frauke Zipp
Journal: Sci Transl Med Date: 2018-02-28 Impact factor: 17.956

6. Functional muscle recovery with nanoparticle-directed M2 macrophage polarization in mice.

Authors: Theresa M Raimondo; David J Mooney
Journal: Proc Natl Acad Sci U S A Date: 2018-10-01 Impact factor: 11.205

7. Macrophage-Derived Vascular Endothelial Growth Factor-A Is Integral to Neuromuscular Junction Reinnervation after Nerve Injury.

Authors: Chuieng-Yi Lu; Katherine B Santosa; Albina Jablonka-Shariff; Bianca Vannucci; Anja Fuchs; Isaiah Turnbull; Deng Pan; Matthew D Wood; Alison K Snyder-Warwick
Journal: J Neurosci Date: 2020-11-06 Impact factor: 6.167

IL-4 expressing cells are recruited to nerve after injury and promote regeneration.

1. IL-4 acts as a myoblast recruitment factor during mammalian muscle growth.

2. Macrophages Regulate Schwann Cell Maturation after Nerve Injury.

Review 3. The multicellular complexity of peripheral nerve regeneration.

4. The CCL2/CCR2 axis is critical to recruiting macrophages into acellular nerve allograft bridging a nerve gap to promote angiogenesis and regeneration.

5. Fast direct neuronal signaling via the IL-4 receptor as therapeutic target in neuroinflammation.

6. Functional muscle recovery with nanoparticle-directed M2 macrophage polarization in mice.

7. Macrophage-Derived Vascular Endothelial Growth Factor-A Is Integral to Neuromuscular Junction Reinnervation after Nerve Injury.

8. A critical role for macrophages near axotomized neuronal cell bodies in stimulating nerve regeneration.

Review 9. Advances in the repair of segmental nerve injuries and trends in reconstruction.

10. Liposomes embedded within fibrin gels facilitate localized macrophage manipulations within nerve.

1. Combined spinal and general anesthesia attenuate tumor promoting effects of surgery. An experimental animal study.