Title: Leuprorelin / Leuprolide Acetate
Post by cluster on Jan 9th, 2011 at 3:28pm
Quote:Leuprorelin as therapy of chronic cluster headache
refractory to conventional prophylactic therapies
and deep brain stimulation: open label observation
M. Nicolodi 1,2
1 Interuniversity Centre of Neurochemistry and Clinical Pharmacology
of Idiopathic Headache, Siena University, Siena, Italy;
2 Foundation Prevention and Therapy Primary Pain and Headache,
Florence, Italy
Aim To treat intractable chronic cluster.
Subjects and procedure Cluster headache (CH), an extremely
painful syndrome may be refractory to therapies as carbolithium,
verapamil, corticosteroids, topiramate and gabapentin. In com-
pletely refractory sufferers Deep Brain Stimulation (DBS) was
used. The present observation included Group A: 67 (66 males, 1
females, mean age 42.4 ± 3.2SD) chronic CH sufferers (attacks
n = 3-6/day, duration 35-67 min) previously unsuccessfully treated
with mentioned prophylactic medication and Group B: 4 (2
females, age 29-58) chronic cluster headache sufferers (attacks
n = 7-11/ day, duration 47-110 min) previously unsuccessfully
treated with prophylactic medications and DBS. All the enrolled
subjects showed an acute abortive drug abuse: Sumatriptan in
Group A (60-80 mg/s.c/day) or Tramadol (1500 ± 5.50 SD)
sometimes (38% of the days) associated with Sumatriptan (24-
42 mg/s.c/day/) in Group B. Leuprorelin 11,75 mg was given once
a month in Group A, five times/month in Group B. The treatment
duration in Group A was 2-3 months (mean 2.1 ± 1.0 SD). Fifty%
relief was achieved during the first 14 days.
Results and conclusion The benefit consisted in a complete relief
for a period of 10-15 months (mean 12.1 months ± 3.2SD), fol-
lowing, 18 suffers had a relapse with 2-4 attacks/ day which
disappeared in a week following 1 injection of leuprorelin. The
other patients had no relapse during the following 4 years. Dif-
ferently Group B need more frequent administration: 5 vials/month.
Nevertheless, following 6 months they have no more than 0-4
attacks/month (mean 2.8 ± 1.9 SD) versus 7-11/ month . They also
use no more tramadol nor abuse sumatriptan. Patients did not
reported serious adverse effects; there is no drop-out. In males,
deficit of sexual desire was abolished by concomitant use of tes-
tosterone 50 mg/day/orally.
Source: Nicolodi M.: „Leuprorelin as therapy of chronic cluster headache refractory to conventional prophylactic therapies and deep brain stimulation: open label observation.“ In: "Abstracts of the 2nd European Headache and Migraine Trust International Congress (EHMTIC). October 28-31, 2010. Nice, France". J Headache Pain 11 (Suppl 1): S35. October 2010. START PRINTPAGEMultimedia File Viewing and Clickable Links are available for Registered Members only!! You need to  or  END PRINTPAGE – Free full text, see PDF page 35. |
|
Summary in plain English: 67 chronic CH sufferers (attacks n = 3-6/day, duration 35-67 min) previously unsuccessfully treated with lithium, verapamil, corticosteroids, topiramate and gabapentin became completely pain free after 2 – 3 injections with Leuprorelin 11,75 mg. 49 of these 67 chronic CH sufferers have been completely pain free for more than 4 years. 18 of these 67 sufferers had a relapse 10-15 months after the treatment with 2-4 attacks/day which disappeared in a week following 1 injection of leuprorelin. Please see START PRINTPAGEMultimedia File Viewing and Clickable Links are available for Registered Members only!! You need to or END PRINTPAGE for more information about the substance. There was a successful RCT with a single injection of 3.75 mg leuprorelin = leuprolide acetate published in 1993: Nicolodi M, Sicuteri F, Poggioni M (August 1993). "Hypothalamic modulation of nociception and reproduction in cluster headache. I. Therapeutic trials of leuprolide". Cephalalgia 13 (4): 253–7. Abstract here: START PRINTPAGEMultimedia File Viewing and Clickable Links are available for Registered Members only!! You need to or END PRINTPAGE Some of the results of this RCT from the full text: Quote:…
Sixty male outpatients suffering from chronic CH who attended the Cluster Headache Unit of the Headache Centre of the University of Florence were asked to participate in the study. The diagnosis was made according to the clinical criteria of the International Headache Society (IHS) (22). The patients had been suffering from CH for at least five years. Exclusion criteria were: systemic diseases, treatment with neuroleptics or antidepressive drugs, age under 21. All the patients were partially refractory to lithium therapy which had not induced an over than 35% improvement in CH.
...
Results - Therapeutic trial
None of the subjects dropped out of the study. Baseline intensity, number of attacks and age of the patients were not statistically different between the leuprolide- and the placebo-treated groups. Placebo treatment did not cause any significant decrease in the mean basal values of either the number of attacks (2.1 ± 0.5 SEM) or the pain intensity (100%) throughout the treatment period (Fig. 1). Neither was any change in the course of CH pattern reported during the follow-up period.
The maximum effect induced by leuprolide was a 63% decrease of the pain intensity (Fig. 2) reported during the third 10 day period after leuprolide administration. The lowest mean frequency of CH crises occurred (0.37) at this time (Fig. 2). The therapeutic effect of leuprolide began after an average of 10.1 days (range 7-15). Twelve of 30 patients who received leuprolide reported resolution of pain 17 days after drug administration. Leuprolide had no effect in 4 of 30 subjects. Fifteen of the leuprolide-treated subjects reported a general benefit which increased over time. A decrease of analgesic consumption approximately mirrored the decrease in both pain intensity and attack frequency. The mean duration of the attacks decreased from 94 min/day (range 40-150 min) to 9.4 min/day (range 0-60 min), which was the mean duration recorded during the third 10 day period after leuprolide depot. There were no differences of treatment response among age groups or patients with moderate or severe pain.
The main side effect of the active treatment was a significant decrease of libido (66% on average), in comparison with the basal situation. In six of the patients treated with leuprolide the decrease of libido was minor (30% decrease in comparison with the basal values). Two of these six patients reported limited benefit of therapy (30% and 40% respectively), one reported a complete resolution of pain and three reported gradual decrease of up to 60% in pain severity. Overall, no consistent relationship between libido and pain pattern was noted. During the follow-up month the benefit produced by leuprolide persisted in 21 out of the 26 subjects who had significantly improved after active drugs. The mean duration of improvement was 3.25 months (range 1-7) Because current prophylactic treatment significantly decreases in effect during successive administrations, leuprolide was administered again to patients who had improved but relapsed. The second period of leuprolide therapy induced an amelioration similar to that of the first Gn-RH agonist administration. |
|
Does anybody here have some personal (good or bad) experience with the Leuprorelin treatment?
|