Limitations in transplantation of astroglia-biomatrix bridges to stimulate corticospinal axon regrowth across large spinal lesion gaps

• Published in: Neuroscience letters Vol. 400; no. 3; pp. 208 - 212
• Main Authors: Deumens, Ronald, Koopmans, Guido C., Honig, Wiel M.M., Maquet, Véronique, Jérôme, Robert, Steinbusch, Harry W.M., Joosten, Elbert A.J.
• Format: Journal Article Web Resource
• Language: English
• Published: Shannon Elsevier Ireland Ltd 12.06.2006; Elsevier
• Subjects: Alignment; Animals; Astrocytes - transplantation; Axons - pathology; Biocompatible Materials - chemistry; Biological and medical sciences; biomaterial; Biomimetic Materials - chemistry; Chemistry; Chimie; Corticospinal; Development. Senescence. Regeneration. Transplantation; Engineering, computing & technology; Extracellular Matrix - chemistry; Fundamental and applied biological sciences. Psychology; Ingénierie, informatique & technologie; Locomotion; Male; Materials science & engineering; Nerve Regeneration - physiology; Physical, chemical, mathematical & earth Sciences; Physique, chimie, mathématiques & sciences de la terre; Polyesters - chemistry; Polylactides; Pyramidal Tracts - growth & development; Pyramidal Tracts - injuries; Rat; Rats; Rats, Inbred Lew; scaffold; Science des matériaux & ingénierie; Spinal Cord Injuries - diagnosis; Spinal Cord Injuries - physiopathology; Spinal Cord Injuries - surgery; Spinal cord injury; Thoracic Vertebrae - injuries; Tissue Engineering - methods; Treatment Outcome; Vertebrates: nervous system and sense organs; Locomotion; Alignment; Polylactides; Rat; Spinal cord injury; Corticospinal; Spinal cord; Rodentia; Central nervous system; Axon; Corticospinal bundle; Transplantation; Vertebrata; Mammalia; Pyramidal motor pathway; Animal; Lesion; Motricity
• ISSN: 0304-3940; 1872-7972; 1872-7972
• DOI: 10.1016/j.neulet.2006.02.050

Regrowth of injured axons across rather small spinal cord lesion gaps and subsequent functional recovery has been obtained after many interventions. Long-distance regeneration of injured axons across clinically relevant large spinal lesion gaps is relatively unexplored. Here, we aimed at stimulating long-distance regrowth of the injured corticospinal (CS) tract. During development, an oriented framework of immature astrocytes is important for correct CS axon outgrowth. Furthermore, a continuous growth promoting substrate may be needed to maintain a CS axon regrowth response across relatively large spinal lesion gaps. Hence, we acutely transplanted poly( d, l)-lactide matrices, which after seeded with immature astrocytes render aligned astrocyte-biomatrix complexes (R. Deumens, et al. Alignment of glial cells stimulates directional neurite growth of CNS neurons in vitro. Neuroscience 125 (3) (2004) 591–604), into 2-mm long dorsal hemisection lesion gaps. In order to create a growth promoting continuum, astrocyte suspensions were also injected rostral and caudal to the lesion gap. During 2 months, locomotion was continuously monitored. Histological analysis showed that astrocytes injected into host spinal tissue survived, but did not migrate. None of the astrocytes on the biomatrices survived within the lesion gap. BDA-labeled CS axons did not penetrate the graft. However, directly rostral to the lesion gap, 120.9 ± 38.5% of the BDA-labeled CS axons were present in contrast to 12.8 ± 3.9% in untreated control animals. The observed anatomical changes were not accompanied by locomotor improvements as analyzed with the BBB and CatWalk. We conclude that although multifactorial strategies may be needed to stimulate long-distance CS axon regrowth, future studies should focus on enhancing the viability of cell/biomatrix complexes within large spinal lesion gaps.