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      Macrophage Transcriptional Profile Identifies Lipid Catabolic Pathways That Can Be Therapeutically Targeted after Spinal Cord Injury

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          Abstract

          Although infiltrating macrophages influence many pathological processes after spinal cord injury (SCI), the intrinsic molecular mechanisms that regulate their function are poorly understood. A major hurdle has been dissecting macrophage-specific functions from those in other cell types as well as understanding how their functions change over time. Therefore, we used the RiboTag method to obtain macrophage-specific mRNA directly from the injured spinal cord in mice and performed RNA sequencing to investigate their transcriptional profile. Our data show that at 7 d after SCI, macrophages are best described as foam cells, with lipid catabolism representing the main biological process, and canonical nuclear receptor pathways as their potential mediators. Genetic deletion of a lipoprotein receptor, CD36, reduces macrophage lipid content and improves lesion size and locomotor recovery. Therefore, we report the first macrophage-specific transcriptional profile after SCI and highlight the lipid catabolic pathway as an important macrophage function that can be therapeutically targeted after SCI.

          SIGNIFICANCE STATEMENT The intrinsic molecular mechanisms that regulate macrophage function after spinal cord injury (SCI) are poorly understood. We obtained macrophage-specific mRNA directly from the injured spinal cord and performed RNA sequencing to investigate their transcriptional profile. Our data show that at 7 d after SCI, macrophages are best described as foam cells, with lipid catabolism representing the main biological process and canonical nuclear receptor pathways as their potential mediators. Genetic deletion of a lipoprotein receptor, CD36, reduces macrophage lipid content and improves lesion size and locomotor recovery. Therefore, we report the first macrophage-specific transcriptional profile after SCI and highlight the lipid catabolic pathway as an important macrophage function that can be therapeutically targeted after SCI.

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          Author and article information

          Journal
          Journal ID (nlm-ta): J Neurosci
          Journal ID (iso-abbrev): J. Neurosci
          Journal ID (hwp): jneuro
          Journal ID (pmc): jneurosci
          Journal ID (publisher-id): J. Neurosci
          Title: The Journal of Neuroscience
          Publisher: Society for Neuroscience
          ISSN (Print): 0270-6474
          ISSN (Electronic): 1529-2401
          Publication date (Print): 1 March 2017
          Publication date PMC-release: 1 September 2017
          Volume: 37
          Issue: 9
          Pages: 2362-2376
          Affiliations
          [1] 1Miami Project to Cure Paralysis, Department of Neurological Surgery, School of Medicine and
          [2] 2Center for Computational Science, University of Miami, Miami, Florida 33136 and
          [3] 3School of Biomedical Engineering, Science and Health Systems, Drexel University, Philadelphia, Pennsylvania 19104
          Author notes
          Correspondence should be addressed to Dr. Jae K. Lee, University of Miami School of Medicine, Miami Project to Cure Paralysis, Department of Neurological Surgery, 1095 Northwest 14th Terrace, LPLC 4-19, Miami, FL 33136. jlee22@ 123456med.miami.edu

          Author contributions: Y. Zhu, K.L., D.H.L., D.M., N.M.F., S.Y., C.S., J.Z., J.R.B., K.L.S., V.P.L., and J.K.L. designed research; Y. Zhu, K.L., D.H.L., D.M., N.M.F., Y. Zhang, S.Y., C.S., J.Z., and J.K.L. performed research; D.M. contributed unpublished reagents/analytic tools; Y. Zhu, K.L., D.H.L., D.M., N.M.F., Y. Zhang, S.Y., C.S., J.Z., K.L.S., and J.K.L. analyzed data; Y. Zhu, K.L., N.M.F., J.R.B., K.L.S., V.P.L., and J.K.L. wrote the paper.

          *Y. Zhu and K.L. contributed equally to this work.

          J. Zha and J. R. Bethea's present address: Department of Biology, Drexel University, Philadelphia, PA 19104.

          Author information
          http://orcid.org/0000-0001-7413-9783
          Article
          Accession ID: PMC5354348 Pmcid ID: PMC5354348 Pmc-uid ID: 5354348 Publisher ID: 2751-16
          DOI: 10.1523/JNEUROSCI.2751-16.2017
          PMC ID: 5354348
          PubMed ID: 28130359
          SO-VID: fb737620-dfc5-4503-9df0-ad9e83e84b10
          Copyright © Copyright © 2017 the authors 0270-6474/17/372362-15$15.00/0
          History
          Date received : 31 August 2016
          Date revision received : 13 January 2017
          Date accepted : 22 January 2017
          Categories
          Subject: Research Articles
          Subject: Development/Plasticity/Repair

          Keywords: foamy macrophages,fibrotic scar,glial scar,myelin laden macrophages,neuroinflammation,axon regeneration
          Data availability:
          Keywords: foamy macrophages, fibrotic scar, glial scar, myelin laden macrophages, neuroinflammation, axon regeneration

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