TY - JOUR
T1 - Communicating hydrocephalus in adult rats with kaolin obstruction of the basal cisterns or the cortical subarachnoid space
AU - Li, Jie
AU - McAllister, James P.
AU - Shen, Yimin
AU - Wagshul, Mark E.
AU - Miller, Janet M.
AU - Egnor, Michael R.
AU - Johnston, Miles G.
AU - Haacke, E. Mark
AU - Walker, Marion L.
N1 - Funding Information:
The authors thank Kelley A. Deren, BS for the administrative support and Joseph E. Madsen, MD, Gary S. Krause, MD, Curtis Stewart, Steven D. Ham, DO, Sandeep Sood, MD, and Holly Gilmer-Hill for their constructive criticism and encouragement. This project was funded by the BrainChild Foundation, Cave Creek, AZ.
PY - 2008/6
Y1 - 2008/6
N2 - Communicating hydrocephalus (CH) occurs frequently, but clinically-relevant animal models amenable to diagnostic imaging and cerebrospinal fluid shunting are not available. In order to develop and characterize models of subarachnoid space (SAS) obstruction at the basal cisterns (BC) or cerebral convexities (CX), 25% kaolin was injected in adult female Sprague-Dawley rats following halothane anesthesia; intact- or saline-injected animals served as controls. For BC animals (n = 28 hydrocephalics, n = 20 controls), an anterior approach to the C1-clivus interval was employed and 30 μl of kaolin or saline was injected. For CX injections (n = 13 hydrocephalics, n = 3 controls), 50-60 μl of kaolin was injected bilaterally after separating the partitions in the SAS. In BC-injected rats, kaolin was observed grossly in the basal cisterns but not in the cisterna magna or at the foramina of Luschka, indicating that communicating (or extra-ventricular) - not obstructive - hydrocephalus had been induced. Following ketamine/xylazine anesthesia, magnetic resonance imaging (MRI) of gadolinium injected into the lateral ventricle also demonstrated CSF flow from the foramina of Luschka. MRI also revealed that ventriculomegaly progressed steadily in BC animals and by 2 weeks post-kaolin the mean Evan's ratio (frontal horn) increased significantly (mean 0.45 compared to 0.31 in intact- and 0.34 in saline-injected controls; p < 0.001 for each). CX animals exhibited kaolin deposits covering approximately 80% of the cerebral hemispheres and developed noticeable ventriculomegaly (mean Evan's ratio 0.40), which was significant relative to intact animals (p = 0.011) but not saline-injected controls. Surprisingly, ventriculomegaly following CX injections was less severe and much more protracted, requiring 3-4 months to develop compared to ventriculomegaly produced by BC obstruction. No hydrocephalic animals demonstrated obvious neurological deficits, but BC-injected animals that subsequently developed more severe ventriculomegaly exhibited nasal discharges and "coughing" for several days following kaolin injection. The new BC model is relevant because the clinical presentation of CH in children is often associated with obstruction at this site, while the CX model may be more representative of late adult onset normal pressure hydrocephalus.
AB - Communicating hydrocephalus (CH) occurs frequently, but clinically-relevant animal models amenable to diagnostic imaging and cerebrospinal fluid shunting are not available. In order to develop and characterize models of subarachnoid space (SAS) obstruction at the basal cisterns (BC) or cerebral convexities (CX), 25% kaolin was injected in adult female Sprague-Dawley rats following halothane anesthesia; intact- or saline-injected animals served as controls. For BC animals (n = 28 hydrocephalics, n = 20 controls), an anterior approach to the C1-clivus interval was employed and 30 μl of kaolin or saline was injected. For CX injections (n = 13 hydrocephalics, n = 3 controls), 50-60 μl of kaolin was injected bilaterally after separating the partitions in the SAS. In BC-injected rats, kaolin was observed grossly in the basal cisterns but not in the cisterna magna or at the foramina of Luschka, indicating that communicating (or extra-ventricular) - not obstructive - hydrocephalus had been induced. Following ketamine/xylazine anesthesia, magnetic resonance imaging (MRI) of gadolinium injected into the lateral ventricle also demonstrated CSF flow from the foramina of Luschka. MRI also revealed that ventriculomegaly progressed steadily in BC animals and by 2 weeks post-kaolin the mean Evan's ratio (frontal horn) increased significantly (mean 0.45 compared to 0.31 in intact- and 0.34 in saline-injected controls; p < 0.001 for each). CX animals exhibited kaolin deposits covering approximately 80% of the cerebral hemispheres and developed noticeable ventriculomegaly (mean Evan's ratio 0.40), which was significant relative to intact animals (p = 0.011) but not saline-injected controls. Surprisingly, ventriculomegaly following CX injections was less severe and much more protracted, requiring 3-4 months to develop compared to ventriculomegaly produced by BC obstruction. No hydrocephalic animals demonstrated obvious neurological deficits, but BC-injected animals that subsequently developed more severe ventriculomegaly exhibited nasal discharges and "coughing" for several days following kaolin injection. The new BC model is relevant because the clinical presentation of CH in children is often associated with obstruction at this site, while the CX model may be more representative of late adult onset normal pressure hydrocephalus.
KW - Basal cisterns
KW - Cerebral ventricles
KW - Communicating hydrocephalus
KW - Hydrocephalus
KW - Kaolin
KW - Magnetic resonance imaging
KW - Rat
KW - Subarachnoid space
UR - https://www.scopus.com/pages/publications/43449112042
U2 - 10.1016/j.expneurol.2007.12.030
DO - 10.1016/j.expneurol.2007.12.030
M3 - Article
C2 - 18433747
AN - SCOPUS:43449112042
SN - 0014-4886
VL - 211
SP - 351
EP - 361
JO - Experimental Neurology
JF - Experimental Neurology
IS - 2
ER -