Laura Vivas scite author profile

The lamina terminalis, located in the anterior wall of the third ventricle, is comprised of the subfornical organ, median preoptic nucleus (MnPO) and organum vasculosum of the lamina terminalis (OVLT). The subfornical organ and OVLT are two of the brain's circumventricular organs that lack the blood-brain barrier, and are therefore exposed to the ionic and hormonal environment of the systemic circulation. Previous investigations in sheep and rats show that this region of the brain has a crucial role in osmoregulatory vasopressin secretion and thirst. The effects of lesions of the lamina terminalis, studies of immediate-early gene expression and electrophysiological data show that all three regions of the lamina terminalis are involved in osmoregulation. There is considerable evidence that physiological osmoreceptors subserving vasopressin release are located in the dorsal cap region of the OVLT and possibly also around the periphery of the subfornical organ and in the MnPO. The circulating peptide hormones angiotensin II and relaxin also have access to peptide specific receptors (AT(1) and LGR7 receptors, respectively) in the subfornical organ and OVLT, and both angiotensin II and relaxin act on the subfornical organ to stimulate water drinking in the rat. Studies that combined neuroanatomical tracing and detection of c-fos expression in response to angiotensin II or relaxin suggest that both of these circulating peptides act on neurones within the dorsal cap of the OVLT and the periphery of the subfornical organ to stimulate vasopressin release.

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The Extended Amygdala and Salt Appetite

Johnson

Olmos

Pastuskovas

et al. 1999

Annals of the New York Academy of Sciences

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Both chemo- and mechanosensitive receptors are involved in detecting changes in the signals that reflect the status of body fluids and of blood pressure. These receptors are located in the systemic circulatory system and in the sensory circumventricular organs of the brain. Under conditions of body fluid deficit or of marked changes in fluid distribution, multiple inputs derived from these humoral and neural receptors converge on key areas of the brain where the information is integrated. The result of this central processing is the mobilization of homeostatic behaviors (thirst and salt appetite), hormone release, autonomic changes, and cardiovascular adjustments. This review discusses the current understanding of the nature and role of the central and systemic receptors involved in the facilitation and inhibition of thirst and salt appetite and on particular components of the central neural network that receive and process input derived from fluid- and cardiovascular-related sensory systems. Special attention is paid to the structures of the lamina terminalis, the area postrema, the lateral parabrachial nucleus, and their association with the central nucleus of the amygdala and the bed nucleus of the stria terminalis in controlling the behaviors that participate in maintaining body fluid and cardiovascular homeostasis.

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Chapter 51: Efferent neural pathways of the lamina terminalis subserving osmoregulation

McKinley

Bicknell

Hards

et al. 1992

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Sodium appetite and Fos activation in serotonergic neurons

Franchini

Johnson

Olmos

et al. 2002

American Journal of Physiology-Regulatory, Integrative and Comp

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2000.-We evaluated serotonergic hindbrain groups of cells for their involvement in the generation and inhibition of sodium appetite. For that purpose, we analyzed the number of Fos-immunoreactive (Fos-ir) cells and double-labeled Fosserotonin (5-HT)-ir neurons within different nuclei of the hindbrain raphe system and the area postrema (AP). Sodium depletion and sodium appetite were induced by peritoneal dialysis. Twenty-four hours after peritoneal dialysis, a 2% NaCl solution intake test was given to peritoneal dialyzed animals [PD-with access (PD-A) group] and to control dialyzed animals [CD-with access (CD-A) group]. Two additional groups of animals received either peritoneal dialysis or control dialysis but were not given access to the 2% NaCl [CD-no access (CD-NA) group or PD-no access (PD-NA) group]. The number of Fos-ir neurons within different nuclei of the raphe system was increased in spontaneous and induced sodium ingestion of CD-A and PD-A groups compared with the CD-NA and PD-NA groups. The PD-NA group had significantly fewer double-labeled cells along the raphe system compared with the animals in near-normal sodium balance (CD-NA and CD-A) or in the process of restoring sodium balance by consuming NaCl (PD-A). The AP of the PD-A group showed a significant increase in the number of Fos-ir and Fos-5-HT-ir cells compared with the PD-NA and CD groups. Our results suggest that serotonergic pathways with cell bodies in the AP and the raphe system are involved in the control of sodium appetite.Fos-serotonin immunoreactivity; area postrema; raphe system RECENTLY, there has been increased interest in identifying the neural network subserving sodium appetite. Forebrain structures such us the circumventricular organs (CVOs) of the lamina terminalis, the organum vasculosum of the lamina terminalis, and the subfornical organ have been identified as key targets processing angiotensin-, osmotic-, and sodium-related information involved in the control of sodium appetite.A hindbrain system has also been recently implicated in the inhibitory control of sodium appetite. This system includes the neural circuitry of the area postrema (AP), nucleus of the solitary tract (NTS), and lateral parabrachial nucleus (LPBN). Ablation of the AP and the immediately adjacent medial NTS (mNTS) increases induced and ad libitum sodium intake (7, 9, 16). Electrolytic or chemical lesions of the LPBN, which receives afferent projections from the AP/mNTS, also enhance drinking induced by intracerebroventricular ANG II as well as other ANG II-related stimuli (10,28,29). Several studies suggest that a serotonergic hindbrain circuit including the LPBN may normally exert an inhibitory action on several models of reninangiotensin-dependent sodium and water intake (6,22,23; see Ref. 18 for review). In addition, previous evidence has indicated that there are central serotonergic influences on sodium and water intake and excretion (24,27,34,37).Serotonergic neurons are located within several nuclei in the midbrain and the brain stem and have dif...

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Laura Vivas

Vasopressin Secretion: Osmotic and Hormonal Regulation by the Lamina Terminalis

The Extended Amygdala and Salt Appetite

Chapter 51: Efferent neural pathways of the lamina terminalis subserving osmoregulation

Sodium appetite and Fos activation in serotonergic neurons

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