Your search keyword '"Vollesen, Anne Luise H"' showing total 7 results

1. The effect of pituitary adenylate cyclase-activating peptide-38 and vasoactive intestinal peptide in cluster headache

Author

Vollesen, Anne Luise H., Snoer, Agneta, Chaudhry, Basit, Petersen, Anja Sofie, Hagedorn, Andreas, Hoffmann, Jan, Jensen, Rigmor H., Ashina, Messoud, Vollesen, Anne Luise H., Snoer, Agneta, Chaudhry, Basit, Petersen, Anja Sofie, Hagedorn, Andreas, Hoffmann, Jan, Jensen, Rigmor H., and Ashina, Messoud

Abstract

Background: Previously reported increases in serum levels of vasodilating neuropeptides pituitary adenylate cyclase-activating peptide-38 (PACAP38) and vasoactive intestinal peptide (VIP) during attacks of cluster headache could indicate their involvement in cluster headache attack initiation. We investigated the attack-inducing effects of PACAP38 and vasoactive intestinal peptide in cluster headache, hypothesising that PACAP38, but not vasoactive intestinal peptide, would induce cluster-like attacks in episodic active phase and chronic cluster headache patients. Methods: In a double-blind crossover study, 14 episodic cluster headache patients in active phase, 15 episodic cluster headache patients in remission phase and 15 chronic cluster headache patients were randomly allocated to receive intravenous infusion of PACAP38 (10 pmol/kg/min) or vasoactive intestinal peptide (8 pmol/kg/min) over 20 min on two study days separated by at least 7 days. We recorded headache intensity, incidence of cluster-like attacks, cranial autonomic symptoms and vital signs using a questionnaire (0–90 min). Results: In episodic cluster headache active phase, PACAP38 induced cluster-like attacks in 6/14 patients and vasoactive intestinal peptide induced cluster-like attacks in 5/14 patients (p = 1.000). In chronic cluster headache, PACAP38 and vasoactive intestinal peptide both induced cluster-like attacks in 7/15 patients (p = 0.765). In episodic cluster headache remission phase, neither PACAP38 nor vasoactive intestinal peptide induced cluster-like attacks. Conclusions: Contrary to our hypothesis, attack induction was lower than expected and roughly equal by PACAP38 and vasoactive intestinal peptide in episodic active phase and chronic cluster headache patients, which contradicts the PAC1-receptor as being solely responsible for attack induction. Trial registration: clinicaltrials.gov (identifier NCT03814226).

Published

2020

2. S100B and NSE in Cluster Headache – Evidence for Glial Cell Activation?

Author

Snoer, Agneta H., Vollesen, Anne Luise H., Beske, Rasmus Paulin, Guo, Song, Hoffmann, Jan, Jørgensen, Niklas R., Martinussen, Torben, Ashina, Messoud, Jensen, Rigmor H., Snoer, Agneta H., Vollesen, Anne Luise H., Beske, Rasmus Paulin, Guo, Song, Hoffmann, Jan, Jørgensen, Niklas R., Martinussen, Torben, Ashina, Messoud, and Jensen, Rigmor H.

Abstract

Objective: Neuronal-specific enolase (NSE) and protein S100B have gained considerable interest as the markers of CNS injury, glial cell activation, and/or blood-brain barrier (BBB) disruption. No studies have investigated NSE and S100B in cluster headache (CH), but these biomarkers could contribute to the understanding of CH. Methods: Patients with episodic CH in bout (eCHa), in remission (eCHr), and chronic CH (cCH) were included in this randomized, double-blind, placebo-controlled, 2-way cross-over provocation study carried out at the Danish Headache Center. The primary endpoints included (1) differences of NSE and S100B in between groups (eCHa, eCHr, and cCH) at baseline; (2) differences over time in plasma concentrations of NSE and S100B between patient developing an attack and those who did not; (3) differences in plasma concentrations over time of NSE and S100B between active day and placebo day. Baseline findings were compared to the historical data on migraine patients and healthy controls and presented with means ± SD. Results: Nine eCHa, 9 eCHr, and 13 cCH patients completed the study and blood samples from 11 CGRP-induced CH attacks were obtained. There were no differences in NSE levels between CH groups at baseline, but CH patients in active disease phase had higher levels compared with 32 migraine patients (9.1 ± 2.2 µg/L vs 6.0 ± 2.2 µg/L, P <.0001) and 6 healthy controls (9.1 ± 2.2 µg/L vs 7.3 ± 2.0 µg/L, P =.007). CGRP-infusion caused no NSE changes and, but a slight, non-significant, increase in NSE was seen in patients who reported a CGRP-induced CH attack (2.39 µg/L, 95% Cl [−0.26, 3.85], P =.061). At baseline S100B levels in eCHa patients were higher compared to cCH patients (0.06 ± 0.02 µg/L vs 0.04 ± 0.02 µg/L, P =.018). Infusion of CGRP and CGRP-induced attacks did not change S100B levels. Apart from induced CH-attacks no other adverse events were noted. Conclusions: At baseline eCHa patients had higher S100B plasma levels than cCH patie

Published

2020

3. S100B and NSE in Cluster Headache – Evidence for Glial Cell Activation?

Author

Snoer, Agneta H., Vollesen, Anne Luise H., Beske, Rasmus Paulin, Guo, Song, Hoffmann, Jan, Jørgensen, Niklas R., Martinussen, Torben, Ashina, Messoud, Jensen, Rigmor H., Snoer, Agneta H., Vollesen, Anne Luise H., Beske, Rasmus Paulin, Guo, Song, Hoffmann, Jan, Jørgensen, Niklas R., Martinussen, Torben, Ashina, Messoud, and Jensen, Rigmor H.

Abstract

Objective: Neuronal-specific enolase (NSE) and protein S100B have gained considerable interest as the markers of CNS injury, glial cell activation, and/or blood-brain barrier (BBB) disruption. No studies have investigated NSE and S100B in cluster headache (CH), but these biomarkers could contribute to the understanding of CH. Methods: Patients with episodic CH in bout (eCHa), in remission (eCHr), and chronic CH (cCH) were included in this randomized, double-blind, placebo-controlled, 2-way cross-over provocation study carried out at the Danish Headache Center. The primary endpoints included (1) differences of NSE and S100B in between groups (eCHa, eCHr, and cCH) at baseline; (2) differences over time in plasma concentrations of NSE and S100B between patient developing an attack and those who did not; (3) differences in plasma concentrations over time of NSE and S100B between active day and placebo day. Baseline findings were compared to the historical data on migraine patients and healthy controls and presented with means ± SD. Results: Nine eCHa, 9 eCHr, and 13 cCH patients completed the study and blood samples from 11 CGRP-induced CH attacks were obtained. There were no differences in NSE levels between CH groups at baseline, but CH patients in active disease phase had higher levels compared with 32 migraine patients (9.1 ± 2.2 µg/L vs 6.0 ± 2.2 µg/L, P <.0001) and 6 healthy controls (9.1 ± 2.2 µg/L vs 7.3 ± 2.0 µg/L, P =.007). CGRP-infusion caused no NSE changes and, but a slight, non-significant, increase in NSE was seen in patients who reported a CGRP-induced CH attack (2.39 µg/L, 95% Cl [−0.26, 3.85], P =.061). At baseline S100B levels in eCHa patients were higher compared to cCH patients (0.06 ± 0.02 µg/L vs 0.04 ± 0.02 µg/L, P =.018). Infusion of CGRP and CGRP-induced attacks did not change S100B levels. Apart from induced CH-attacks no other adverse events were noted. Conclusions: At baseline eCHa patients had higher S100B plasma levels than cCH patie

Published

2020

4. S100B and NSE in cluster headache -evidence for glial cell activation?

Author

Snoer, Agneta, Vollesen, Anne Luise H., Beske, Rasmus P., Guo, Song, Hoffmann, Jan, Fahrenkrug, Jan, Joergesen, Niklas R., Martinussen, Torben, Jensen, Rigmor H., Ashina, Messoud, Snoer, Agneta, Vollesen, Anne Luise H., Beske, Rasmus P., Guo, Song, Hoffmann, Jan, Fahrenkrug, Jan, Joergesen, Niklas R., Martinussen, Torben, Jensen, Rigmor H., and Ashina, Messoud

Published

2019

5. S100B and NSE in cluster headache -evidence for glial cell activation?

Author

Snoer, Agneta, Vollesen, Anne Luise H., Beske, Rasmus P., Guo, Song, Hoffmann, Jan, Fahrenkrug, Jan, Joergesen, Niklas R., Martinussen, Torben, Jensen, Rigmor H., Ashina, Messoud, Snoer, Agneta, Vollesen, Anne Luise H., Beske, Rasmus P., Guo, Song, Hoffmann, Jan, Fahrenkrug, Jan, Joergesen, Niklas R., Martinussen, Torben, Jensen, Rigmor H., and Ashina, Messoud

Published

2019

6. Calcitonin-gene related peptide and disease activity in cluster headache

Author

Snoer, Agneta, Vollesen, Anne Luise H., Beske, Rasmus P., Guo, Song, Hoffmann, Jan, Fahrenkrug, Jan, Jørgensen, Niklas Rye, Martinussen, Torben, Jensen, Rigmor H., Ashina, Messoud, Snoer, Agneta, Vollesen, Anne Luise H., Beske, Rasmus P., Guo, Song, Hoffmann, Jan, Fahrenkrug, Jan, Jørgensen, Niklas Rye, Martinussen, Torben, Jensen, Rigmor H., and Ashina, Messoud

Published

2019

7. Calcitonin-gene related peptide and disease activity in cluster headache

Author

Snoer, Agneta, Vollesen, Anne Luise H., Beske, Rasmus P., Guo, Song, Hoffmann, Jan, Fahrenkrug, Jan, Jørgensen, Niklas Rye, Martinussen, Torben, Jensen, Rigmor H., Ashina, Messoud, Snoer, Agneta, Vollesen, Anne Luise H., Beske, Rasmus P., Guo, Song, Hoffmann, Jan, Fahrenkrug, Jan, Jørgensen, Niklas Rye, Martinussen, Torben, Jensen, Rigmor H., and Ashina, Messoud

Published

2019