FK-506 a new immunosuppressive agent, failed to reduce cerebral vasospasm after experimental subarachnoid hemorrhage

To define the relationship between the immunologic reaction and the pathogenesis of cerebral vasospasm (VS) following experimental subarachnoid hemorrhage (SAH), we examined the effect of a cell mediated immunosuppressive agent, FK-506, isolated from Streptomyces tsukubaensis, by using the canine SA...

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Published inJournal of Veterinary Medical Science Vol. 55; no. 4; pp. 581 - 586
Main Authors Mori, T. (Nippon Medical School, Kawasaki, Kanagawa (Japan)), Nagata, K, Ishida, T, Sasaki, T, Nirei, H, Hamada, K, Ohami, H, Kirino, T
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Published Japan JAPANESE SOCIETY OF VETERINARY SCIENCE 01.08.1993
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Abstract To define the relationship between the immunologic reaction and the pathogenesis of cerebral vasospasm (VS) following experimental subarachnoid hemorrhage (SAH), we examined the effect of a cell mediated immunosuppressive agent, FK-506, isolated from Streptomyces tsukubaensis, by using the canine SAH model. There was a significant vasoconstriction in the basilar artery in the control group after SAH. This constriction, however was not successfully prevented by FK-506 or combination of FK-506 and steroid, since there was no significant difference in the vessel caliber size among these groups. The pathologic approach, accompanied by immunohistochemistry, could not discriminate the differences in the nature of the lesion between the untreated group and FK-506 treated groups, except for slight lymphocytic infiltrations present around the basilar artery of untreated group. Histopathologically, inflammatory reactions consisting of neutrophils, that were not suppressed by FK-506 treatment, were clearly seen around the spastic vessels in the subarachnoid space. Furthermore, several constrictive changes or degenerative alterations were also observed in the spastic vascular wall. Immunohistochemically, the deposition of IgG, IgM and C3 was present in the intima and the luminal side of the smooth muscle layer, and capillary vessels of the brain stem. It is considered that this deposition was caused by increased vascular permeability in VS. On the basis of the above findings that the cell mediated immunosuppressive agent, FK-506 failed to prevent vasoconstriction or pathologic lesions but lymphocytic infiltrations, it is considered that the cell mediated immunopathogenesis may play little role in producing VS following SAH.
AbstractList To define the relationship between the immunologic reaction and the pathogenesis of cerebral vasospasm (VS) following experimental subarachnoid hemorrhage (SAH), we examined the effect of a cell mediated immunosuppressive agent, FK-506, isolated from Streptomyces tsukubaensis, by using the canine SAH model. There was a significant vasoconstriction in the basilar artery in the control group after SAH. This constriction, however was not successfully prevented by FK-506 or combination of FK-506 and steroid, since there was no significant difference in the vessel caliber size among these groups. The pathologic approach, accompanied by immunohistochemistry, could not discriminate the differences in the nature of the lesion between the untreated group and FK-506 treated groups, except for slight lymphocytic infiltrations present around the basilar artery of untreated group. Histopathologically, inflammatory reactions consisting of neutrophils, that were not suppressed by FK-506 treatment, were clearly seen around the spastic vessels in the subarachnoid space. Furthermore, several constrictive changes or degenerative alterations were also observed in the spastic vascular wall. Immunohistochemically, the deposition of IgG, IgM and C3 was present in the intima and the luminal side of the smooth muscle layer, and capillary vessels of the brain stem. It is considered that this deposition was caused by increased vascular permeability in VS. On the basis of the above findings that the cell mediated immunosuppressive agent, FK-506 failed to prevent vasoconstriction or pathologic lesions but lymphocytic infiltrations, it is considered that the cell mediated immunopathogenesis may play little role in producing VS following SAH.
To define the relationship between the immunologic reaction and the pathogenesis of cerebral vasospasm (VS) following experimental subarachnoid hemorrhage (SAH), we examined the effect of a cell mediated immunosuppressive agent, FK-506, isolated from Streptomyces tsukubaensis, by using the canine SAH model. There was a significant vasoconstriction in the basilar artery in the control group after SAH. This constriction, however was not successfully prevented by FK-506 or combination of FK-506 and steroid, since there was no significant difference in the vessel caliber size among these groups. The pathologic approach, accompanied by immunohistochemistry, could not discriminate the differences in the nature of the lesion between the untreated group and FK-506 treated groups, except for slight lymphocytic infiltrations present around the basilar artery of untreated group. Histopathologically, inflammatory reactions consisting of neutrophils, that were not suppressed by FK-506 treatment, were clearly seen around the spastic vessels in the subarachnoid space. Furthermore, several constrictive changes or degenerative alterations were also observed in the spastic vascular wall. Immunohistochemically, the deposition of IgG, IgM and C sub(3) was present in the intima and the luminal side of the smooth muscle layer, and capillary vessels of the brain stem. It is considered that this deposition was caused by increased vascular permeability in VS. On the basis of the above findings that the cell mediated immunosuppressive agent, FK-506 failed to prevent vasoconstriction or pathologic lesions by lymphocytic infiltrations, it is considered that the cell mediated immunopathogenesis may play little role in producing VS following SAH. (DBO)
Author Hamada, K
Mori, T. (Nippon Medical School, Kawasaki, Kanagawa (Japan))
Ishida, T
Kirino, T
Nirei, H
Ohami, H
Nagata, K
Sasaki, T
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Ochiai, T., Nagata, M., Nakajima, K., Suzuki, T., Sakamo- to, K., Enomoto, K., Gunji, Y., Uematsu, T., Goto, T., Hori, S., Kenmochi, T., Nakagouri, T., Asano, T., Isono, K., Hamaguchi, K., Tsuchida, H.. Nakahara, K., Inamura, N., and Goto, T. 1987. Studies of the effects of FK506 on renal allografting in the beagle dog. Transplantation 44: 729-733.
Pellettieri, L., Carlsson, C-A., and Lindholm, L. 1981. Is the vasospasm following subarachnoid hemorrhage an immunoreactive disease? Experientia 37: 1170-1171.
Inamura, N., Nakahara, K., Nishio, M., Kino, T., Goto, T., Aoki, H., Yamaguchi, I., Kohsaka, M., and Ochiai, T. 1988. Prolongation of skin allograft survival in rats by a novel immunosuppressive agent, FK-506. Transplantation 45: 206-209.
Peterson, J. W., Nishizawa, S., Hackett, J. D., Bun, T., Teramura, A., and Zervas, N. T. 1990. Cyclosporine A reduces cerebral vasospasm after subarachnoid hemorrhage in dogs. Stroke 21: 133-137.
Sano, K. 1982. Cerebral vasospasm and aneurysm surgery. Clin. Neurosurg. 30: 13-58.
Borel, J. F. 1989. Pharmacology of Cyclosporine (Sandimmune) IV Pharmacological properties in vivo: Pharmacol. Rev. 41: 259-371.
Nakagomi, T., Kassell, N. F., Sasaki, T., Lehman, R. M., and Fujiwara, S. 1990. Etiology of the disruption in blood-arterial wall barrier following experimental subarachnoid hemorrhage. Surg. Neurol. 34: 16-26.
Kino, T., Hatanaka, H., Miyata, S., Inamura, N., Nishiyama, M., Yajima, T., Goto, T., Okuhara, M., Kohsaka, M., Aoki, H., and Ochiai, T. 1987. FK-506, a novel immunosuppressant isolated from a streptomyces II. Immunosuppressive effect of FK506 in vitro. J. Antibiot. 40: 1256-1265.
Rickels, E., Seifert, V., Zumkeller, M., Kunz, U., and Reale, E. 1990. Corrugation of cerebral vessels following subarachnoid hemorrhage: comparison of two experimental models of chronic cerebral vasospasm. Exp. Neurology 107: 178-186.
Sasaki, T., Kassell, N. F., Yamashita, M., Fujiwara, S., and Zuccarello, M. 1985. Barrier disruption in the major cerebral arteries following experimental subarachnoid hemorrhage. J. Neurosurg. 63: 433-440.
Ostergard, J. R., Kristensen, B. O., Svehag, S. E., Teisner, B., and Miletic, T. 1987. Immunecomplexes and complement activation following rupture of intracranial saccular aneurysms. J. Neurosurg. 66: 891-897.
Liszczak, ThM., Black, PMc., Tzouras, A., Foley, L., and Zervas, N. T. 1984. Morphological changes of the basilar artery, ventricles, and choroid plexus after experiemental SAH. J. Neurosurg. 61: 486-493.
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SubjectTerms Animals
Basilar Artery - drug effects
Basilar Artery - physiopathology
BLOOD VESSELS
BRAIN
Brain Stem - pathology
canine
cerebral vasospasm
CEREBRO
CHIEN
DOGS
ENCEPHALE
ESPASMO
EXPERIMENTACION
EXPERIMENTATION
Female
FK-506
HAEMORRHAGE
HEMORRAGIA
HEMORRAGIE
IMMUNODEPRESSEUR
IMMUNOSUPPRESSANTS
INMUNODEPRESORES
Ischemic Attack, Transient - pathology
Ischemic Attack, Transient - physiopathology
Ischemic Attack, Transient - prevention & control
Male
Muscle, Smooth, Vascular - drug effects
Muscle, Smooth, Vascular - pathology
Muscle, Smooth, Vascular - physiopathology
PERRO
SPASME
SPASMS
subarachnoid hemorrhage
Subarachnoid Hemorrhage - complications
Subarachnoid Hemorrhage - pathology
Subarachnoid Hemorrhage - physiopathology
Tacrolimus - pharmacology
VAISSEAU SANGUIN
VASOS SANGUINEOS
Title FK-506 a new immunosuppressive agent, failed to reduce cerebral vasospasm after experimental subarachnoid hemorrhage
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