Reaction of ependymal cells to spinal cord injury: a potential role for oncostatin pathway and microglial cells

Chevreau, Robert; Ghazale, Hussein; Ripoll, Camille; Chalfouh, Chaima; Delarue, Quentin; Hemonnot-Girard, Anne-Laure; Hirbec, Hélène; Wahane, Shalaka; Perrin, Florence E.; Noristani, Harun N.; Guérout, Nicolas; Hugnot, Jean‐Philippe

doi:10.1101/2021.02.12.428106

Cited by 1 publication

(1 citation statement)

References 48 publications

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“…Indeed, this mSCI model allows one to investigate the response of the spinal cord to the traumatic injury with minimal impact of the other pathological processes (e.g., secondary ischemia, extensive edema, or cavitation) at the cellular level directly in the segment containing the lesion site. The abovementioned approach is obvious in several publications on the reaction of the ependymal lining of central canal in the response to various non‐standardized mSCI models (e.g., Barnabé‐Heider et al., 2010; Chevreau et al., 2021; Huang et al., 2018; Li et al., 2016; Mothe & Tator, 2005; Ren et al., 2017). Although the scientific benefits of the results obtained from these studies are unquestionable, because these models are based mostly on manually executed incisions or punctures, their main disadvantage is the impossibility to execute a similar impact in another ontogenetic stage/animal species.…”

Section: Discussionmentioning

confidence: 99%

Comparative model of minimal spinal cord injury reveals a rather anti‐inflammatory response in the lesion site as well as increased proliferation in the central canal lining in the neonates compared to the adult rats

Ševc,

Mochnacký,

Košuth

et al. 2024

Developmental Neurobiology

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Spinal cord injury (SCI) resulting from trauma decreases the quality of human life. Numerous clues indicate that the limited endogenous regenerative potential is a result of the interplay between the inhibitory nature of mature nervous tissue and the inflammatory actions of immune and glial cells. Knowledge gained from comparing regeneration in adult and juvenile animals could draw attention to factors that should be removed or added for effective therapy in adults. Therefore, we generated a minimal SCI (mSCI) model with a comparable impact on the spinal cord of Wistar rats during adulthood, preadolescence, and the neonatal period. The mechanism of injury is based on unilateral incision with a 20 ga needle tip according to stereotaxic coordinates into the dorsal horn of the L4 lumbar spinal segment. The incision should harm a similar amount of gray matter on a coronal section in each group of experimental animals. According to our results, the impact causes mild injury with minimal adverse effects on the neurological functions of animals but still has a remarkable effect on nervous tissue and its cellular and humoral components. Testing the mSCI model in adults, preadolescents, and neonates revealed a rather anti‐inflammatory response of immune cells and astrocytes at the lesion site, as well as increased proliferation in the central canal lining in neonates compared with adult animals. Our results indicate that developing nervous tissue could possess superior reparative potential and confirm the importance of comparative studies to advance in the field of neuroregeneration.

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