Neonatal experiences with ethanol intoxication modify respiratory and thermoregulatory plasticity and affect subsequent ethanol intake in rats

被引:11
|
作者
Belen Acevedo, Maria [1 ]
Fabiola Macchione, Ana [1 ,2 ]
Anunziata, Florencia [1 ]
Beatriz Haymal, Olga [1 ]
Carlos Molina, Juan [1 ,3 ]
机构
[1] Univ Nacl Cordoba, INIMEC CONICET, Inst Invest Med Mercedes & Martin Ferreyra, Friuli 2434, RA-5016 Cordoba, Argentina
[2] Univ Nacl Cordoba, Fac Odontol, Cordoba, Argentina
[3] Univ Nacl Cordoba, Fac Psicol, Cordoba, Argentina
关键词
breathing disruptions; early ethanol intoxication; ethanol; intake rat; neonate; thermoregulation; ALCOHOL SPECTRUM DISORDERS; INFANT-DEATH-SYNDROME; CHEMOSENSORY CUES; INDUCED HYPOTHERMIA; PRENATAL EXPOSURE; DEMONSTRATOR RATS; BRAIN-DEVELOPMENT; PREWEANLING RATS; ADOLESCENT RATS; ANIMAL-MODEL;
D O I
10.1002/dev.21466
中图分类号
Q [生物科学];
学科分类号
07 ; 0710 ; 09 ;
摘要
Different studies have focused on the deleterious consequences of binge-like or chronic exposure to ethanol during the brain growth spurt period (third human gestational trimester) that in the rat corresponds to postnatal days (PDs) 3-10. The present study analyzed behavioral and physiological disruptions caused by relatively brief binge-like exposures (PDs 3, 5, and 7) with an ethanol dose lower (3.0 g/kg) than those frequently employed to examine teratological effects during this stage in development. At PD 9, pups were exposed to ethanol doses ranging between.0-3.0 g/kg and tested in terms of breathing patterns and thermoregulation. At PDs 11 and 12, ethanol intake was examined. The main findings were as follows: i) pre-exposure to the drug resulted in brief depressions in breathing frequencies and an exacerbated predisposition toward apneic episodes; ii) these effects were not dependent upon thermoregulatory alterations; iii) early ethanol treatment increased initial consumption of the drug which also caused a marked hypothermia that appeared to regulate a subsequent decrement in ethanol consumption; and iv) ethanol exposure retarded overall body growth and even one exposure to the drug (PD 9) was sufficient to reduce brain weights although there were no indications of microcephaly. In conjunction with studies performed during the late gestational period in the rat, the results indicate that relatively brief binge-like episodes during a critical window of brain vulnerability disrupts the respiratory network and exacerbates initial acceptance of the drug. In addition, ethanol treatments were not found to induce tolerance relative to respiratory and thermal disruptions.
引用
收藏
页码:48 / 59
页数:12
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