Effect of indomethacin on cerebral blood flow, carbon dioxide reactivity and the response to epoprostenol (prostacyclin) infusion in man.

Pickles, H; Brown, Martin M.; Thomas, Martin; Hewazy, A H; Redmond, S; Zilkha, E.; Marshall, John

doi:10.1136/jnnp.47.1.51

Cited by 26 publications

(13 citation statements)

References 19 publications

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“…In one study no control group received hypercapnia; a significant increase in CBF was seen with a very modest increase in CO 2 concentration from 5.0 to 5.5 kPa, but this may represent a nonspecific response to the stress of the mask and the CO 2 . 13 Furthermore, without a control group it is unclear whether the response to hypercapnia was reduced compared with normal subjects, as the trend in our study suggested, or was unaltered as found by Pickles et al 14 However, other studies revealing conflicting results induced greater changes in end-tidal CO 2 concentrations, similar to those attained in our study, and used ade- Abbreviations as in Table 1. Standard deviations are shown in parentheses.…”

Section: Discussionsupporting

confidence: 64%

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Differential effect of three cyclooxygenase inhibitors on human cerebral blood flow velocity and carbon dioxide reactivity.

Markus

Vallance

Brown

1994

Stroke

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Prostaglandins are believed to play an important role in maintenance of cerebral blood flow and possibly in the vasodilatory response to carbon dioxide. Therefore, the nonsteroidal anti-inflammatory drugs and aspirin, which inhibit cyclooxygenase, might be expected to reduce cerebral blood flow and the response to hypercapnia. This could induce cerebral ischemia in patients with a hemodynamically critical circulation. It would also interfere with the measurement of cerebrovascular reserve using carbon dioxide. The effect of a single dose of indomethacin and of two other cyclooxygenase inhibitors (aspirin and sulindac) on the cerebral circulation was measured using transcranial Doppler ultrasonography of the middle cerebral artery. Seven normal adults were studied in each drug group. Resting blood flow velocity and the responses to hypercapnia and to hyperventilation were measured. Indomethacin resulted in a fall in basal middle cerebral artery flow velocity from a mean of 48.9 cm/s to 34.0 cm/s (P < .002). It also reduced the vasoconstrictor response to hypocapnia (induced by hyperventilation) from 37.5% to 20.7% (P < .003). There was a nonsignificant reduction in the vasodilatory response to 8% carbon dioxide (mean: predrug, 87.7%; postdrug, 61.0%), with marked intersubject variability. In contrast, basal middle cerebral artery velocity and vasoconstrictor and vasodilatory responses to changes in carbon dioxide were unchanged after aspirin or sulindac administration. The lack of effect of aspirin on basal cerebral blood flow velocity and on vasodilatory reserve is reassuring; aspirin will not reduce cerebral blood flow or the response to a reduced perfusion pressure in patients with critically impaired cerebral hemodynamics. However, indomethacin should be avoided in such patients.

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Section: Discussionsupporting

confidence: 64%

“…- 14 In addition, in some animal models indomethacin reduces the cerebral vasodilatory response to hypercapnia, 7 ' 810 although studies in humans have revealed conflicting results.…”

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confidence: 99%

Differential effect of three cyclooxygenase inhibitors on human cerebral blood flow velocity and carbon dioxide reactivity.

Markus

Vallance

Brown

1994

Stroke

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“…1). In contrast, Pickles et al (1984) reported a reduced basal CBF without any concurrent changes in cerebrovascular CO 2 reactivity in six participants following 2 days of INDO oral administration (100 mg day -1 ). However, in that study, participants were given 50 mg of INDO the morning of the experiment, whilst the present and other previous studies (Bruhn et al 2001;Eriksson et al 1983;Fan et al 2010;Ivancev et al 2009;Markus et al 1994;St Lawrence et al 2002;Wennmalm et al 1983;Xie et al 2006Xie et al , 2009 have assessed the effect of INDO on the cerebrovascular CO 2 reactivity following a single larger dose of INDO (100 mg) 90 min prior to measurement.…”

Section: Influence Of Indomethacin On Cerebrovascular Reactivity To Cmentioning

confidence: 77%

“…However, in that study, participants were given 50 mg of INDO the morning of the experiment, whilst the present and other previous studies (Bruhn et al 2001;Eriksson et al 1983;Fan et al 2010;Ivancev et al 2009;Markus et al 1994;St Lawrence et al 2002;Wennmalm et al 1983;Xie et al 2006Xie et al , 2009 have assessed the effect of INDO on the cerebrovascular CO 2 reactivity following a single larger dose of INDO (100 mg) 90 min prior to measurement. Accordingly, these methodological differences make it difficult to compare the findings of the Pickles et al (1984) study. Nishimura et al (1987) have previously found a reduction in the arterial-to-internal venous jugular PCO 2 difference during 5-15 min of hypoxic exposure in healthy humans.…”

Section: Influence Of Indomethacin On Cerebrovascular Reactivity To Cmentioning

confidence: 98%

Influence of indomethacin on the ventilatory and cerebrovascular responsiveness to hypoxia

et al. 2010

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Indomethacin (INDO) has the potential to be a useful tool to explore the influence of cerebral blood flow and its responses to CO(2) on ventilatory control. However, the effect of INDO on the cerebrovascular and ventilatory response to hypoxia remains unclear; therefore, we examined the effect of INDO on ventilatory and cerebrovascular sensitivity to hypoxia and hypercapnia. We measured end-tidal gases, ventilation (V(e)), and middle cerebral artery velocity (MCAv) before and 90 min following INDO (100 mg) in 12 healthy participants at rest and during hyperoxic hypercapnia and isocapnic hypoxia. Following INDO, resting VE and end-tidal gases were unaltered (P > 0.05), whilst MCAv was lowered by 25 ± 19% (P < 0.001). INDO ingestion reduced MCAv-CO(2) reactivity by 46 ± 29% (2.9 ± 0.9 vs. 1.7 ± 0.9 cm s(-1) mmHg(-1); P < 0.001) and enhanced the VE-CO(2) sensitivity by 0.5 ± 0.5 L min(-1) mmHg(-1) (1.9 ± 1.5 vs. 2.3 ± 1.6 L min(-1) mmHg(-1); P < 0.05). No changes were observed in either the MCAv or VE responsiveness to isocapnic hypoxia following INDO ingestion (P > 0.05). These findings indicate that INDO does not alter cerebrovascular and ventilatory responsiveness to hypoxia, indicating a preserved peripheral chemoreflex in response to this pharmacological agent.

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“…In addition, due to the reduction in arterial blood pressure, the net effect of prostacyclin in this study was a reduction in the cerebral perfusion pres sure. Other studies have shown that prostacyclin may cause both a reduction in cerebral blood flow [38] and cerebral perfusion pressure [39]. In this study, prostacyc lin caused a reduction in arterial oxygen tension and for the majority of patients studied a reduction in cardiac output.…”

Section: Discussionmentioning

confidence: 64%

Adverse Effects on Cerebral Perfusion of Prostacyclin Administered Directly into Patients with Fulminant Hepatic Failure and Acute Renal Failure

Davenport¹,

Will²,

Davison³

1991

Nephron

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Prior to commencing renal replacement therapy, 8 patients with fulminant hepatic failure and acute renal failure were treated with an infusion of prostacyclin, 5 ng/kg/min, for 30 min, administered directly into the femoral vein. During this period, several adverse effects were noted. There was a reduction in mean arterial blood pressure from a median of 82 (range 65–93) to 67 mm Hg (55–80), p < 0.01; and an increase in intracranial pressure from a median of 14 (6–33) to 17 mm Hg (6–42), p < 0.05; with a consequent reduction in cerebral perfusion pressure from a median of 63 (43–77) to 43 mm Hg (15–74), p < 0.05. There was a reduction in arterial oxygen tension from a median of 19 (13–28) to 16 kPa (12–27), p < 0.05; and no change in cardiac output, from a median of 6.7 (4.9–11.2) to 6.5 1/min/m² (3.8–11.0), p > 0.05. The administration of prostacyclin into this group of critically ill patients, at risk of death due to cerebral oedema/hypoxia, produced both a reduction in cerebral perfusion pressure and a reduction in total cerebral oxygen delivery.

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Effect of indomethacin on cerebral blood flow, carbon dioxide reactivity and the response to epoprostenol (prostacyclin) infusion in man.

Cited by 26 publications

References 19 publications

Differential effect of three cyclooxygenase inhibitors on human cerebral blood flow velocity and carbon dioxide reactivity.

Differential effect of three cyclooxygenase inhibitors on human cerebral blood flow velocity and carbon dioxide reactivity.

Influence of indomethacin on the ventilatory and cerebrovascular responsiveness to hypoxia

Adverse Effects on Cerebral Perfusion of Prostacyclin Administered Directly into Patients with Fulminant Hepatic Failure and Acute Renal Failure

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