Generation and processing of peripheral temperature signals in mammals

Pierau, Fr.-K.; Wurster, Robert D.; Neya, Toshiaki; Yamasato, Teruhiro; Ulrich, J

doi:10.1007/bf02249793

Cited by 16 publications

(3 citation statements)

References 15 publications

(13 reference statements)

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“…197 1 ;Iriki and Simon 1973) and skin temperature in our experiments. These changes may have stimulated cutaneous thermoreceptors (Hensel 1976;Pierau et al 1980;Sumins and Dubner 1981) to effect the changes in GC that we observed. Increases in central levels of adenosine (Laudignon et al 1991;Phillis et al 1987;VanWylen et al 1986;Ticho and Radulovacki 1991 ;Wang et al-1992) md (or) histamine (Sudhakaran et al 1979;Wada et id.…”

Section: Discussionmentioning

confidence: 68%

Body-core temperature decreases during hypoxic hypoxia in Long–Evans and Brattleboro rats

Clark¹,

Fewell²

1994

Can. J. Physiol. Pharmacol.

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In newborn mammals, hypoxic hypoxia produces a regulated decrease in body-core temperature, the mechanism of which is unknown. Since plasma and cerebrospinal fluid levels of arginine vasopressin increase during hypoxemia and intracerebroventricular administration of arginine vasopressin decreases body-core temperature, it has been hypothesized that an increase in central arginine vasopressin may mediate this response. Experiments were therefore carried out to test the hypothesis that the body-core temperature response to hypoxic hypoxia would be different in Brattleboro rats (which lack arginine vasopressin containing cells in the central nervous system) compared with that observed in Long-Evans rats (which have arginine vasopressin containing cells in the central nervous system). Both mild (15% oxygen) and severe (10% oxygen) hypoxic hypoxia decreased body-core temperature in both strains of rats, the decrease actually being accentuated in the Brattleboro rats. Thus, our data do not support the hypothesis that an increase in central arginine vasopressin mediates the regulated decrease in body-core temperature during hypoxic hypoxia in rats.

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Section: Discussionmentioning

confidence: 68%

Body-core temperature decreases during hypoxic hypoxia in Long–Evans and Brattleboro rats

Clark¹,

Fewell²

1994

Can. J. Physiol. Pharmacol.

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“…Stimulation of the nucleus raphe magnus has no effect on the spinal trigeminal neurones which respond to facial skin temperature (Dawson, Dickenson, Hellon & Woolf, 1981). There is evidence, however, that the scrotal skin temperature responsive neurones in the dorsal horn of the rat 316 SCROTAL THERMAL PATHWA Y AND RAPHE MAGNUS spinal cord are subject to tonic descending control (Pierau, Neya, Yamasato & Ulrich, 1980). Cooling the thoracic spinal cord, which reversibly blocks descending pathways, decreases the intrinsic firing rate of 60% of the scrotal temperature-responsive neurones in the spinal cord but the activity of the remaining temperature-responsive neurones is usually increased.…”

Section: Discussionmentioning

confidence: 99%

The effects of nucleus raphe magnus lesions on an ascending thermal pathway in the rat.

Taylor¹

1982

The Journal of Physiology

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SUMMARY1. In the thalamus and hypothalamus of rats, anaesthetized with Urethane, single unit recordings have been made from cells which respond to small innocuous changes in scrotal skin temperature applied with a water-perfused brass thermode.2. Once a scrotal temperature-sensitive neurone had been isolated the brain stem was electrolytically lesioned through implanted tungsten electrodes to determine whether the input from the scrotal skin temperature sensors ascends through the brain stem lemniscal pathways or the mid-line raphe nuclei. All recording sites and lesions were identified histologically.3. Thirty-six neurones have been studied of which half were located in the ventrobasal thalamus, six were located in the anterior thalamic nuclei and the remainder were in the medial hypothalamus.4. The nucleus raphe magnus was lesioned on eighteen separate occasions; in each case the temperature-responsive activity of the thalamic or hypothalamic neurone was abolished.5. Extensive brain-stem lesions which spared only the mid-line nucleus raphe magnus had no discernible effect on the responses of the thalamic or hypothalamic neurones to scrotal skin temperature.6. The ascending pathway from the thermal sensors of the rat scrotal skin must pass through, or relay in, the nucleus raphe magnus.

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“…Three neurons were identified as inverse warm-reactive because the scrotal skin warming produced an inhibition and the cooling restored the intrinsic activity in the pre-warming period without inducing any facilitation (HELLON and MISRA, 1973a). Figure 3 shows the static activity of 29 neurons of the static and dynamic/ static warm-reactive type as a function of the scrotal temperature.In most of (PIERAU et al,1980).As is demonstrated in Fig.4…”

Section: Temperature Reaction Of Warm-reactive Dhnsmentioning

confidence: 73%

Activity patterns of temperature-reactive dorsal horn neurons and their reactions to peripheral receptor stimulation by Ca.

Neya¹,

Pierau²

1980

Jpn.J.Physiol

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Generation and processing of peripheral temperature signals in mammals

Cited by 16 publications

References 15 publications

Body-core temperature decreases during hypoxic hypoxia in Long–Evans and Brattleboro rats

Body-core temperature decreases during hypoxic hypoxia in Long–Evans and Brattleboro rats

The effects of nucleus raphe magnus lesions on an ascending thermal pathway in the rat.

Activity patterns of temperature-reactive dorsal horn neurons and their reactions to peripheral receptor stimulation by Ca.

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