Inhibition of astrocyte hemichannel improves recovery from spinal cord injury
Chao Zhang, … , Naomi L. Sayre, Jean X. Jiang
Chao Zhang, … , Naomi L. Sayre, Jean X. Jiang
Published March 8, 2021
Citation Information: JCI Insight. 2021;6(5):e134611. https://doi.org/10.1172/jci.insight.134611.
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Research Article Therapeutics

Inhibition of astrocyte hemichannel improves recovery from spinal cord injury

Abstract

Spinal cord injury (SCI) causes severe disability, and the current inability to restore function to the damaged spinal cord leads to lasting detrimental consequences to patients. One strategy to reduce SCI morbidity involves limiting the spread of secondary damage after injury. Previous studies have shown that connexin 43 (Cx43), a gap junction protein richly expressed in spinal cord astrocytes, is a potential mediator of secondary damage. Here, we developed a specific inhibitory antibody, mouse-human chimeric MHC1 antibody (MHC1), that inhibited Cx43 hemichannels, but not gap junctions, and reduced secondary damage in 2 incomplete SCI mouse models. MHC1 inhibited the activation of Cx43 hemichannels in both primary spinal astrocytes and astrocytes in situ. In both SCI mouse models, administration of MHC1 after SCI significantly improved hind limb locomotion function. Remarkably, a single administration of MHC1 30 minutes after injury improved the recovery up to 8 weeks post-SCI. Moreover, MHC1 treatment decreased gliosis and lesion sizes, increased white and gray matter sparing, and improved neuronal survival. Together, these results suggest that inhibition of Cx43 hemichannel function after traumatic SCI reduces secondary damage, limits perilesional gliosis, and improves functional recovery. By targeting hemichannels specifically with an antibody, this study provides a potentially new, innovative therapeutic approach in treating SCI.

Authors

Chao Zhang, Zhao Yan, Asif Maknojia, Manuel A. Riquelme, Sumin Gu, Grant Booher, David J. Wallace, Viktor Bartanusz, Akshay Goswami, Wei Xiong, Ningyan Zhang, Michael J. Mader, Zhiqiang An, Naomi L. Sayre, Jean X. Jiang

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Figure 5

Blocking Cx43 hemichannel function by MHC1 antibody decreases spinal cord gliosis and protects neuron survival under the model 1 impact.

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Blocking Cx43 hemichannel function by MHC1 antibody decreases spinal cor...
Spinal cords were isolated 14 days or 56 days after the model 1 impact of SCI treated with IgG control or MHC1 antibody. (A) The frozen sections were immunolabeled with anti-MAP2 or anti-GFAP antibody and counterstained with DAPI. The representative images of MAP2 and GFAP immunofluorescence were shown from the perilesion areas. (B) The quantification of MAP2-positive signals by NIH ImageJ software. SCI+IgG 14D (n = 3), SCI+MHC1 14D (n = 3), SCI+IgG 56D (n = 3), SCI+MHC1 56D (n = 3). (C) The quantification of GFAP-positive signals by NIH ImageJ software. SCI+IgG 14D (n = 3), SCI+MHC1 14D (n = 3), SCI+IgG 56D (n = 3), SCI+MHC1 56D (n = 4). All images were taken from perilesional area, which is confined to 1.5 mm from injury border of sagittal sections. The white dotted lines label the lesion border. Scale bar: 50 μm. Data are presented as mean ± SEM. Unpaired t test (1 tailed) was used in statistical analysis. **P < 0.01.