| Literature DB >> 26634814 |
Beatriz Paniagua-Torija1, Angel Arevalo-Martin1, Isidro Ferrer2, Eduardo Molina-Holgado1, Daniel Garcia-Ovejero1.
Abstract
Cannabinoids are involved in the regulation of neural stem cell biology and their receptors are expressed in the neurogenic niches of adult rodents. In the spinal cord of rats and mice, neural stem cells can be found in the ependymal region, surrounding the central canal, but there is evidence that this region is largely different in adult humans: lacks a patent canal and presents perivascular pseudorosettes, typically found in low grade ependymomas. Using Laser Capture Microdissection, Taqman gene expression assays and immunohistochemistry, we have studied the expression of endocannabinoid system components (receptors and enzymes) at the human spinal cord ependymal region. We observe that ependymal region is enriched in CB1 cannabinoid receptor, due to high CB1 expression in GFAP+ astrocytic domains. However, in human spinal cord levels that retain central canal patency we found ependymal cells with high CB1 expression, equivalent to the CB1(HIGH) cell subpopulation described in rodents. Our results support the existence of ependymal CB1(HIGH) cells across species, and may encourage further studies on this subpopulation, although only in cases when central canal is patent. In the adult human ependyma, which usually shows central canal absence, CB1 may play a different role by modulating astrocyte functions.Entities:
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Year: 2015 PMID: 26634814 PMCID: PMC4669459 DOI: 10.1038/srep17745
Source DB: PubMed Journal: Sci Rep ISSN: 2045-2322 Impact factor: 4.379
Relative expression of endocannabinoid system related genes in the adult human ependymal region compared with ventral horn.
| Δ | ΔC | ||||
|---|---|---|---|---|---|
| CNR2 | – | – | – | ||
| GPR55 | – | ||||
| DAGLA | 2,34 | 0,8 | |||
| DAGLB | 14,6 | 0,51 | |||
| MGLL | 0,25 | 0,44 | |||
| ABHD6 | 1,48 | 0,75 | |||
| ABHD12 | 4,7 | 0,095 | |||
| NAPEPLD | – | ||||
| FAAH | – |
*Significantly enriched in Ependymal region vs Ventral Horn (Student T-test).
#ND: Non detected in the Ependymal region of any individual; NCD: Non consistently detected (detected in less than 3 of the 4 individuals).
Figure 1CB1 cannabinoid receptor in adult human spinal cord.
(A) Myelin staining of a representative thoracic spinal cord section. Square depicts the area shown in (C–E). (B) In low magnification a strong CB1 immunoreactivity can be found in dorsal horn, lamina X and ventral gray matter. (C–E) Higher magnification of central gray shows CB1 expression in GFAP+ areas surrounding the Vimentin+ cells at the ependymary region (EpR). Square highlights the location of a perivascular pseudorosette (PvPR). (F–J) Strong CB1 immunoreactivity is found at the GFAP+ domains around and inside perivascular pseudorosettes, including the GFAP ribbon at the hypocellular region of the pseudorosette (hcr, outlined in white). In PvPRs cells are arranged around a central vessel ((I) arrow). (K) Quantification supports qualitative observations: CB1 immunoreactivity is significantly accumulated in GFAP+ areas. (L) Detail of the dorsal aspect of an ependymal region with a patent central canal. Square depicts location of images M and N. (M) CB1HIGH ependymal cells (empty arrows) can be found intermingled with ependymocytes lining the central canal. GFAP+ cells contacting central canal lumen (arrowhead) are CB1−. (N) Detail of M, showing a CB1HIGH cell with a dim staining of GFAP in the apical region. ***T student, p < 0.001; CC, Central Canal; EpR, ependymal region; hcr, hypocellular region; PvPR, perivascular pseudorosette; WM, white matter. Scale bars: A,B = 1 mm; C-E: 100 μm; F-L = 50 μm; M,N = 25 μm.
Figure 2CB1 immunoreactivity can be found in astrocytes of other regions in the spinal cord.
(A–F) CB1 is expressed in the processes of GFAP+ and Vim+ astrocytes (arrows) at the dorsolateral white matter. (G–I) A strong CB1 expression can be found in astrocytic processes at the subpial region. Scale bars: 25 μm.
Postmortem Spinal Cord tissue samples used for immunohistochemistry (IHC) and/or Laser Capture Microdissection (LCMD).
| Autopsy number | Cause of Death | Gender | Age | Coded as | Postmortem delay | Used for |
|---|---|---|---|---|---|---|
| BC01015 | Unknown. No significant neuropathological alterations in the spinal cord | Male | 60 | Control | Unknown | IHC |
| BC01684 | Acute Hypoxia-ischemia | Male | 27 | Control | Unknown | IHC |
| A07/00044 | Cardiopulmonary arrest | Male | 39 | Control | 3 h 30 min | IHC |
| A07/00067 | Refractary septic shock and cardiac arrest. Ischemic cardiopathy | Male | 47 | Control | 4 h 55 min | IHC |
| A10/00017 | Hepatic metastasis. Probable pancreatic neoplasia | Male | 52 | Control | 03 h | IHC |
| A07/00041 | Multiorganic failure. Gastric tumour | Male | 43 | Control | 5 h 55 min | IHC, LCMD |
| A07/00084 | Refractary septic shock | Male | 46 | Control | 15 h | IHC, LCMD |
| A10/00026 | Multiorganic failure. Severe broncopathy | Male | 61 | Control | 3 h 55 min | LCMD |
| A05/00134 | Carcinoma and metastasis. With brain but not spinal cord metastasis. | Female | 32 | Control | 11 h 45 m | LCMD |
| A11/00052 | Endocarditis. No neuropathological features | Male | 76 | Control | 06 h 30 m | LCMD |
| A12/00046 | Cardiac arrest. No neuropathological features | Female | 75 | Control | 06 h10 m | LCMD |