Drug-induced Hypothermia by 5HT1A Agonists Provide Neuroprotection in Experimental Stroke: New Perspectives for Acute Patient Treatment

Flemming Fryd Johansen; Henrik Hasseldam; Matthias Nybro Smith; Rune Skovgaard Rasmussen

doi:10.1016/j.jstrokecerebrovasdis.2014.07.019

Drug-induced Hypothermia by 5HT1A Agonists Provide Neuroprotection in Experimental Stroke: New Perspectives for Acute Patient Treatment

Flemming Fryd Johansen, Henrik Hasseldam, Matthias Nybro Smith, Rune Skovgaard Rasmussen

15 Citationer (Scopus)

Abstract

BACKGROUND: Drug-induced hypothermia reduces brain damage in animal stroke models and is an undiscovered potential in human stroke treatment. We studied hypothermia induced by the serotonergic agonists S14671 (1-[2-(2-thenoylamino)ethyl]-4[1-(7- methoxynaphtyl)]piperazine) and ipsapirone in a rat stroke model and in man by literature meta-analysis.

METHODS: Rats had 60 minutes of middle cerebral artery occlusion (MCAO) and then 7 days of survival. Body temperatures were monitored for 22 hours. Thirty minutes after MCAO, 1 group (n = 9) received bolus of S14671 (.75 mg/kg) and continuous infusion of .06 mg/kg hour(-1) S14671 for 20 hours. Other MCAO rats (n = 7) had bolus of ipsapirone (.75 mg/kg) and continuous infusion of .25 mg/kg hour(-1) ipsapirone for 3 hours. Controls (n = 9; n = 5) received similar amounts of vehicle as bolus and continuous infusion for 20 hours/3 hours. Additional controls of the S14761 effect in MCAO were performed as previously mentioned (n = 10) but with rats kept normothermic by a heating lamp for 22 hours. Finally, a meta-analysis of ipsapirone-induced hypothermia in man was included.

RESULTS: Infarct volumes were reduced by 50% in hypothermic rats versus controls (P < .05). S14671 rats kept normothermic did not show infarct reduction (P > .05). The body temperature after stroke was reduced 1.0-3.0°C compared with controls for 20 hours with S14671 treatment and for 6 hours with ipsapirone treatment. In humans, ipsapirone reduced temperature in average with .55°C ranging between .1-1.4°C.

CONCLUSIONS: 5-hydroxytryptamine receptor 1A (5HT1A) agonists significantly reduce infarct volumes in MCAO rats primarily because of the hypothermic drug effect. 5HT1A agonists may be introduced to reduce body temperatures rapidly and prepare patients for further therapeutic hypothermia.

Originalsprog	Engelsk
Tidsskrift	Journal of Stroke & Cerebrovascular Diseases
Vol/bind	23
Udgave nummer	10
Sider (fra-til)	2879-2887
Antal sider	9
ISSN	1052-3057
DOI	https://doi.org/10.1016/j.jstrokecerebrovasdis.2014.07.019
Status	Udgivet - 9 okt. 2014

Adgang til dokumentet

10.1016/j.jstrokecerebrovasdis.2014.07.019

Citationsformater

Drug-induced Hypothermia by 5HT1A Agonists Provide Neuroprotection in Experimental Stroke : New Perspectives for Acute Patient Treatment. / Johansen, Flemming Fryd; Hasseldam, Henrik; Nybro Smith, Matthias et al.

I: Journal of Stroke & Cerebrovascular Diseases, Bind 23, Nr. 10, 09.10.2014, s. 2879-2887.

Publikation: Bidrag til tidsskrift › Tidsskriftartikel › Forskning › peer review

@article{857e8185917142e0b8e9ffe5848ad020,

title = "Drug-induced Hypothermia by 5HT1A Agonists Provide Neuroprotection in Experimental Stroke: New Perspectives for Acute Patient Treatment",

abstract = "BACKGROUND: Drug-induced hypothermia reduces brain damage in animal stroke models and is an undiscovered potential in human stroke treatment. We studied hypothermia induced by the serotonergic agonists S14671 (1-[2-(2-thenoylamino)ethyl]-4[1-(7- methoxynaphtyl)]piperazine) and ipsapirone in a rat stroke model and in man by literature meta-analysis.METHODS: Rats had 60 minutes of middle cerebral artery occlusion (MCAO) and then 7 days of survival. Body temperatures were monitored for 22 hours. Thirty minutes after MCAO, 1 group (n = 9) received bolus of S14671 (.75 mg/kg) and continuous infusion of .06 mg/kg hour(-1) S14671 for 20 hours. Other MCAO rats (n = 7) had bolus of ipsapirone (.75 mg/kg) and continuous infusion of .25 mg/kg hour(-1) ipsapirone for 3 hours. Controls (n = 9; n = 5) received similar amounts of vehicle as bolus and continuous infusion for 20 hours/3 hours. Additional controls of the S14761 effect in MCAO were performed as previously mentioned (n = 10) but with rats kept normothermic by a heating lamp for 22 hours. Finally, a meta-analysis of ipsapirone-induced hypothermia in man was included.RESULTS: Infarct volumes were reduced by 50% in hypothermic rats versus controls (P < .05). S14671 rats kept normothermic did not show infarct reduction (P > .05). The body temperature after stroke was reduced 1.0-3.0°C compared with controls for 20 hours with S14671 treatment and for 6 hours with ipsapirone treatment. In humans, ipsapirone reduced temperature in average with .55°C ranging between .1-1.4°C.CONCLUSIONS: 5-hydroxytryptamine receptor 1A (5HT1A) agonists significantly reduce infarct volumes in MCAO rats primarily because of the hypothermic drug effect. 5HT1A agonists may be introduced to reduce body temperatures rapidly and prepare patients for further therapeutic hypothermia.",

author = "Johansen, {Flemming Fryd} and Henrik Hasseldam and {Nybro Smith}, Matthias and Rasmussen, {Rune Skovgaard}",

year = "2014",

month = oct,

day = "9",

doi = "10.1016/j.jstrokecerebrovasdis.2014.07.019",

language = "English",

volume = "23",

pages = "2879--2887",

journal = "Journal of Stroke & Cerebrovascular Diseases",

issn = "1052-3057",

publisher = "W.B.Saunders Co.",

number = "10",

}

TY - JOUR

T1 - Drug-induced Hypothermia by 5HT1A Agonists Provide Neuroprotection in Experimental Stroke

T2 - New Perspectives for Acute Patient Treatment

AU - Johansen, Flemming Fryd

AU - Hasseldam, Henrik

AU - Nybro Smith, Matthias

AU - Rasmussen, Rune Skovgaard

PY - 2014/10/9

Y1 - 2014/10/9

N2 - BACKGROUND: Drug-induced hypothermia reduces brain damage in animal stroke models and is an undiscovered potential in human stroke treatment. We studied hypothermia induced by the serotonergic agonists S14671 (1-[2-(2-thenoylamino)ethyl]-4[1-(7- methoxynaphtyl)]piperazine) and ipsapirone in a rat stroke model and in man by literature meta-analysis.METHODS: Rats had 60 minutes of middle cerebral artery occlusion (MCAO) and then 7 days of survival. Body temperatures were monitored for 22 hours. Thirty minutes after MCAO, 1 group (n = 9) received bolus of S14671 (.75 mg/kg) and continuous infusion of .06 mg/kg hour(-1) S14671 for 20 hours. Other MCAO rats (n = 7) had bolus of ipsapirone (.75 mg/kg) and continuous infusion of .25 mg/kg hour(-1) ipsapirone for 3 hours. Controls (n = 9; n = 5) received similar amounts of vehicle as bolus and continuous infusion for 20 hours/3 hours. Additional controls of the S14761 effect in MCAO were performed as previously mentioned (n = 10) but with rats kept normothermic by a heating lamp for 22 hours. Finally, a meta-analysis of ipsapirone-induced hypothermia in man was included.RESULTS: Infarct volumes were reduced by 50% in hypothermic rats versus controls (P < .05). S14671 rats kept normothermic did not show infarct reduction (P > .05). The body temperature after stroke was reduced 1.0-3.0°C compared with controls for 20 hours with S14671 treatment and for 6 hours with ipsapirone treatment. In humans, ipsapirone reduced temperature in average with .55°C ranging between .1-1.4°C.CONCLUSIONS: 5-hydroxytryptamine receptor 1A (5HT1A) agonists significantly reduce infarct volumes in MCAO rats primarily because of the hypothermic drug effect. 5HT1A agonists may be introduced to reduce body temperatures rapidly and prepare patients for further therapeutic hypothermia.

AB - BACKGROUND: Drug-induced hypothermia reduces brain damage in animal stroke models and is an undiscovered potential in human stroke treatment. We studied hypothermia induced by the serotonergic agonists S14671 (1-[2-(2-thenoylamino)ethyl]-4[1-(7- methoxynaphtyl)]piperazine) and ipsapirone in a rat stroke model and in man by literature meta-analysis.METHODS: Rats had 60 minutes of middle cerebral artery occlusion (MCAO) and then 7 days of survival. Body temperatures were monitored for 22 hours. Thirty minutes after MCAO, 1 group (n = 9) received bolus of S14671 (.75 mg/kg) and continuous infusion of .06 mg/kg hour(-1) S14671 for 20 hours. Other MCAO rats (n = 7) had bolus of ipsapirone (.75 mg/kg) and continuous infusion of .25 mg/kg hour(-1) ipsapirone for 3 hours. Controls (n = 9; n = 5) received similar amounts of vehicle as bolus and continuous infusion for 20 hours/3 hours. Additional controls of the S14761 effect in MCAO were performed as previously mentioned (n = 10) but with rats kept normothermic by a heating lamp for 22 hours. Finally, a meta-analysis of ipsapirone-induced hypothermia in man was included.RESULTS: Infarct volumes were reduced by 50% in hypothermic rats versus controls (P < .05). S14671 rats kept normothermic did not show infarct reduction (P > .05). The body temperature after stroke was reduced 1.0-3.0°C compared with controls for 20 hours with S14671 treatment and for 6 hours with ipsapirone treatment. In humans, ipsapirone reduced temperature in average with .55°C ranging between .1-1.4°C.CONCLUSIONS: 5-hydroxytryptamine receptor 1A (5HT1A) agonists significantly reduce infarct volumes in MCAO rats primarily because of the hypothermic drug effect. 5HT1A agonists may be introduced to reduce body temperatures rapidly and prepare patients for further therapeutic hypothermia.

U2 - 10.1016/j.jstrokecerebrovasdis.2014.07.019

DO - 10.1016/j.jstrokecerebrovasdis.2014.07.019

M3 - Journal article

C2 - 25307429

SN - 1052-3057

VL - 23

SP - 2879

EP - 2887

JO - Journal of Stroke & Cerebrovascular Diseases

JF - Journal of Stroke & Cerebrovascular Diseases

IS - 10

ER -

Drug-induced Hypothermia by 5HT1A Agonists Provide Neuroprotection in Experimental Stroke: New Perspectives for Acute Patient Treatment

Abstract

Adgang til dokumentet

Fingeraftryk

Citationsformater