Vasopressin serum levels in patients with severe brain lesions and in brain-dead patients

Cintra, Eliane de Araújo; Maciel, Jayme Antunes; Araújo, Sebastião; Castro, Margaret de; Martins, Edna Freitas; Falcão, Antônio Luís Eiras; Sardinha, Luiz Antônio; Terzi, Renato Giuseppe Giovanni; Dragosavac, Desanka; Cardoso, Ana Paula Devite; Oliveira, Rosmari Aparecida Rosa Almeida de

doi:10.1590/s0004-282x2004000200007

Cited by 11 publications

(11 citation statements)

References 21 publications

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“…Chen et al [21] reported plasma AVP levels varying from 2.2 to 8.0 pg/mL in normovolemic patients and normotensive patients, with serum osmolarity ≤ 290 mOsm/L. In a previous study of our group [22], plasma AVP values in 29 healthy adults individuals at rest were also very low (ranging from 0.4 to 5.2 pg/mL).= In the present investigation, preoperative (T0 -basal period) mean plasma AVP levels were of 1.37±0.73 pg/mL (median=1.34 pg/mL; range=0.30 -3.1 pg/mL), thus, inside those previously described by our group [22] in healthy resting adult individuals.…”

Section: Time Course Of Vasopressin In Our Patientsmentioning

confidence: 63%

Vasopressina plasmática em pacientes submetidos à correção de aneurisma de aorta infrarrenal

Carvalho¹,

Guillaumon²,

Cintra³

et al. 2011

Rev Bras Cir Cardiovasc

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Objectives: To evaluate plasmatic arginine vasopressin (AVP) levels in patients undergoing scheduled conventional abdominal aortic aneurysm (AAA) repair.Methods: Plasmatic AVP concentrations were measured by radioimmunoassay in 22 non-consecutive adult patients undergoing infra-renal AAA repair. They were under combined general and epidural anesthesia at the following time frames: 1 -pre-operative (T0); 2 -2h (T1) and 6h (T2) after the surgical procedure; 3 -in the morning at the first (T3), second (T4) and third (T5) post-operative days. Some clinical and laboratory variables were also recorded.Results: The mean age of patients was 68±10 years; 17 were males. Plasmatic AVP (mean±SD; pg/mL) was within the normal range at T0 (1.4±0.7; baseline), increasing significantly at T1 (62.6±62.9; P<0.001) and at T2 (31.5±49.7; P<0.001), with a progressive fall, returning to basal levels at T5 (2.1±3.8; P=NS). Positive and statistically significant correlations were found between AVP and glycemia, serum lactate and white blood cells counts, but not with systemic arterial pressure or plasma osmolarity during the postoperative period.Conclusions: Considering that no correlations were found between AVP levels and hemodynamic or plasmatic osmolarity variations in AAA repair, it seems that stress response is mainly secondary to noxious stimulation mediated by the autonomic nervous system that is not completely blocked by anesthetics. Descriptors: Intensive care units. Cardiovascular abnormalities. Receptors, vasopressin. Resumo Objetivos: Avaliar os níveis plasmáticos de vasopressina (AVP) em pacientes submetidos à correção convencional de aneurisma de aorta abdominal (AAA).Métodos: A AVP plasmática foi mensurada por radioimunoensaio em 22 pacientes não-consecutivos submetidos à correção eletiva de AAA infrarrenal sob anestesia geral + epidural nos seguintes momentos: pré-operatório (T0); 2h (T1) e 6h (T2) após a cirurgia; e nas manhãs do primeiro (T3), segundo (T4) e terceiro (T5) dia pós-operatório (PO). Variáveis clínicas e laboratoriais de interesse também foram anotadas.Resultados: A média de idade dos pacientes foi de 68±10 anos, sendo 17 homens. A AVP plasmática (média±DP; pg/ mL) estava dentro de limites normais no T0 (1,4±0,7; basal), aumentando no T1 (62,6±62,9; P<0,001) e no T2 (31,5±49,7; P<0,001), e retornando aos valores basais no T5 (2,1±3,8; RBCCV 44205-1296

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Section: Time Course Of Vasopressin In Our Patientsmentioning

confidence: 63%

Vasopressina plasmática em pacientes submetidos à correção de aneurisma de aorta infrarrenal

Carvalho¹,

Guillaumon²,

Cintra³

et al. 2011

Rev Bras Cir Cardiovasc

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“…Most importantly, however, several experimental and clinical studies already demonstrated that vasopressin is involved in brain edema formation. Elevated vasopressin serum levels were found in patients suffering from brain edema due to brain tumors (Tenedieva et al, 1994), subarachnoidal hemorrhage (Mather et al, 1981), cerebral ischemia (Barreca et al, 2001), or TBI (Huang et al, 2003;Cintra et al, 2004). Although ICV or intravenous application of arginine vasopressin in experimental animals does not cause swelling of normal brain (Vajda et al, 2001), it increases brain edema formation following pathological conditions, for example, cortical cold lesion (Reeder et al, 1986) or cerebral ischemia (Liu et al, 1996).…”

Section: Discussionmentioning

confidence: 99%

“…Several studies indicate that patients with traumatic brain injury (TBI), subarachnoid hemorrhage, or cerebral ischemia have increased AVP levels in plasma and cerebrospinal fluid (Mather et al, 1981;Joynt et al, 1981;Cintra et al, 2004;Xu et al, 2007). Similarly, studies in rats showed an increased expression of V 1 receptor levels after experimental TBI (Szmydynger-Chodobska et al, 2004;Pascale et al, 2006).…”

Section: Introductionmentioning

confidence: 99%

Role of Vasopressin V_1a and V₂ Receptors for the Development of Secondary Brain Damage after Traumatic Brain Injury in Mice

Trabold

Krieg

Schöller

et al. 2008

Journal of Neurotrauma

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Brain edema is still one of the most deleterious sequels of traumatic brain injury (TBI), and its pathophysiology is not sufficiently understood. The goal of the current study was to investigate the role of arginine vasopressin (AVP), also known as antidiuretic hormone (ADH), an important regulator of tissue water homeostasis, for the formation of post-traumatic brain edema, intracranial pressure (ICP), brain damage, and functional deficits following brain trauma. C57/B16 mice (n=112) were subjected to controlled cortical impact (CCI; 8m/s, 1 mm). At 3 min after trauma, animals received 500 ng of the AVP V(1a)-receptor antogonist (deamino-Pen(1), O-Me-Tyr(2), Arg(8)]-Vasopressin) or 500 ng of the AVP V2-receptor antagonist (adamantaneacetyl(1), O-Et-D-Tyr(2),Val(4), Abu(6),Arg(8,9)]-Vasopressin) by intracerebroventricular injection. After trauma, cerebral water content (24 h), ICP (24 h), contusion volume (24 h and 7 days), and functional outcome (1-7 days) were assessed (n=8 per experimental group). Post-traumatic inhibition of AVP V(1A) receptors reduced ICP by 29% (p < 0.05), brain water content by 45% (p < 0.05), and secondary contusion expansion by 37% (p < 0.05), and it significantly improved motor function 6 and 7 days after trauma (p < 0.05). Inhibition of AVP V2 receptors had no significant effect. The current results demonstrate that vasopressin V(1A) receptors are involved in the pathogenesis of brain edema formation and the subsequent development of secondary brain damage after traumatic brain injury. Accordingly, our study suggests that vasopressin V(1A) receptors may represent a novel therapeutic target for the treatment of post-traumatic brain edema and secondary brain damage.

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“…[38][39][40] Barreca and colleagues reported elevated serum AVP levels that were independent of osmo-and baro-mechanisms in post-ischemic human conditions. 41 In addition, elevated AVP levels in the cerebral spinal fluid (CSF) were found specifically in neurological disorders that have increased intracranial pressure.…”

Section: Animal Modelmentioning

confidence: 99%

Arginine Vasopressin V_1a Receptor-Deficient Mice Have Reduced Brain Edema and Secondary Brain Damage following Traumatic Brain Injury

Rauen¹,

Trabold²,

Brem³

et al. 2013

Journal of Neurotrauma

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The formation of brain edema and subsequent intracranial hypertension are major predictors of unfavorable outcome following traumatic brain injury (TBI). Previously, we reported that arginine vasopressin (AVP) receptor antagonists reduce post-traumatic and post-ischemic brain edema in mice. The aim of the current study was to investigate further the contribution of arginine vasopressin V1a receptors to TBI-induced secondary brain damage in V1a receptor knock-out mice. V1a receptor knock-out (V1a -/-) and wild-type mice were subjected to controlled cortical impact (CCI), and edema (brain water content measured before and 24 h after CCI), primary and secondary contusion volume (15 min and 24 h after CCI), neurological function (one day before and seven days after CCI), body weight (before and seven days after CCI) and mortality were measured. Twenty-four h after CCI, V1a receptor knock-out mice had significantly less brain water content than wild-type mice (mean±standard error of the mean: 79.8%±0.3 vs. 80.6%±0.2, respectively), and secondary contusion volume was significantly smaller (38.2±1.7 mm(3) vs. 45.1±1.5 mm(3) in wild-type mice). Furthermore, the V1a receptor knock-out mice had less neurological dysfunction (3.2±0.8 vs. 7.0±1.4 in wild-type mice) and weight loss (1.0±1.0% vs. 4.9±1.8% in wild-type mice) seven days after CCI. Our data show that mice lacking V1a receptors have less secondary brain damage following experimental traumatic brain injury. We therefore conclude that V1a receptors may represent a novel drug target for preventing post-traumatic brain edema.

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Vasopressin serum levels in patients with severe brain lesions and in brain-dead patients

Cited by 11 publications

References 21 publications

Vasopressina plasmática em pacientes submetidos à correção de aneurisma de aorta infrarrenal

Vasopressina plasmática em pacientes submetidos à correção de aneurisma de aorta infrarrenal

Role of Vasopressin V_1a and V₂ Receptors for the Development of Secondary Brain Damage after Traumatic Brain Injury in Mice

Arginine Vasopressin V_1a Receptor-Deficient Mice Have Reduced Brain Edema and Secondary Brain Damage following Traumatic Brain Injury

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Vasopressin serum levels in patients with severe brain lesions and in brain-dead patients

Cited by 11 publications

References 21 publications

Vasopressina plasmática em pacientes submetidos à correção de aneurisma de aorta infrarrenal

Vasopressina plasmática em pacientes submetidos à correção de aneurisma de aorta infrarrenal

Role of Vasopressin V1a and V2 Receptors for the Development of Secondary Brain Damage after Traumatic Brain Injury in Mice

Arginine Vasopressin V1a Receptor-Deficient Mice Have Reduced Brain Edema and Secondary Brain Damage following Traumatic Brain Injury

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Role of Vasopressin V_1a and V₂ Receptors for the Development of Secondary Brain Damage after Traumatic Brain Injury in Mice

Arginine Vasopressin V_1a Receptor-Deficient Mice Have Reduced Brain Edema and Secondary Brain Damage following Traumatic Brain Injury