Intravenous clomipramine challenge in obsessive-compulsive disorder: predicting response to oral therapy at eight weeks
Background: Challenge with intravenous clomipramine (CMI) is serotonin selective and has been reported to transiently exacerbate symptoms in obsessive-compulsive disorder (OCD) patients, and to predict subsequent response to oral CMI therapy. Methods: We administered CMI (12.5 mg, IV) to medication...
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Published in | Biological psychiatry (1969) Vol. 44; no. 3; pp. 220 - 227 |
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Main Authors | , , , , |
Format | Journal Article |
Language | English |
Published |
New York, NY
Elsevier Inc
01.08.1998
Elsevier Science |
Subjects | |
Online Access | Get full text |
ISSN | 0006-3223 1873-2402 |
DOI | 10.1016/S0006-3223(97)00373-9 |
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Abstract | Background: Challenge with intravenous clomipramine (CMI) is serotonin selective and has been reported to transiently exacerbate symptoms in obsessive-compulsive disorder (OCD) patients, and to predict subsequent response to oral CMI therapy.
Methods: We administered CMI (12.5 mg, IV) to medication free OCD patients (
N = 29) and normal controls (
N = 22) to characterize neurohormonal response. A subset of OCD patients (26/29), was then treated with either pulse load IV or oral CMI followed by 8 weeks of oral CMI therapy.
Results: In response to CMI challenge, OCD patients exhibit blunted cortisol and exaggerated growth hormone response relative to normal controls. OCD patients differ from controls in “sadness” ratings, with controls exhibiting increased dysphoria in response to CMI. Growth hormone response to CMI challenge predicts treatment response (≥ 25% ↓ YBOCS from baseline) to oral CMI at 8 weeks.
Conclusions: Growth hormone abnormalities associated with OCD in response to CMI challenge differentiates nonresponders after 8 weeks of oral CMI treatment from responders. |
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AbstractList | Background: Challenge with intravenous clomipramine (CMI) is serotonin selective and has been reported to transiently exacerbate symptoms in obsessive-compulsive disorder (OCD) patients, and to predict subsequent response to oral CMI therapy.
Methods: We administered CMI (12.5 mg, IV) to medication free OCD patients (
N = 29) and normal controls (
N = 22) to characterize neurohormonal response. A subset of OCD patients (26/29), was then treated with either pulse load IV or oral CMI followed by 8 weeks of oral CMI therapy.
Results: In response to CMI challenge, OCD patients exhibit blunted cortisol and exaggerated growth hormone response relative to normal controls. OCD patients differ from controls in “sadness” ratings, with controls exhibiting increased dysphoria in response to CMI. Growth hormone response to CMI challenge predicts treatment response (≥ 25% ↓ YBOCS from baseline) to oral CMI at 8 weeks.
Conclusions: Growth hormone abnormalities associated with OCD in response to CMI challenge differentiates nonresponders after 8 weeks of oral CMI treatment from responders. Challenge with intravenous clomipramine (CMI) is serotonin selective and has been reported to transiently exacerbate symptoms in obsessive-compulsive disorder (OCD) patients, and to predict subsequent response to oral CMI therapy. We administered CMI (12.5 mg, i.v.) to medication free OCD patients (N = 29) and normal controls (N = 22) to characterize neurohormonal response. A subset of OCD patients (26/29), was then treated with either pulse load i.v. or oral CMI followed by 8 weeks of oral CMI therapy. In response to CMI challenge, OCD patients exhibit blunted cortisol and exaggerated growth hormone response relative to normal controls. OCD patients differ from controls in "sadness" ratings, with control exhibiting increased dysphoria in response to CMI. Growth hormone response to CMI challenge predicts treatment response (> or = 25% decreases YBOCS from baseline) to oral CMI at 8 weeks. Growth hormone abnormalities associated with OCD in response to CMI challenge differentiates nonresponders after 8 weeks of oral CMI treatment from responders. Challenge with intravenous clomipramine (CMI) is serotonin selective and has been reported to transiently exacerbate symptoms in obsessive-compulsive disorder (OCD) patients, and to predict subsequent response to oral CMI therapy.BACKGROUNDChallenge with intravenous clomipramine (CMI) is serotonin selective and has been reported to transiently exacerbate symptoms in obsessive-compulsive disorder (OCD) patients, and to predict subsequent response to oral CMI therapy.We administered CMI (12.5 mg, i.v.) to medication free OCD patients (N = 29) and normal controls (N = 22) to characterize neurohormonal response. A subset of OCD patients (26/29), was then treated with either pulse load i.v. or oral CMI followed by 8 weeks of oral CMI therapy.METHODSWe administered CMI (12.5 mg, i.v.) to medication free OCD patients (N = 29) and normal controls (N = 22) to characterize neurohormonal response. A subset of OCD patients (26/29), was then treated with either pulse load i.v. or oral CMI followed by 8 weeks of oral CMI therapy.In response to CMI challenge, OCD patients exhibit blunted cortisol and exaggerated growth hormone response relative to normal controls. OCD patients differ from controls in "sadness" ratings, with control exhibiting increased dysphoria in response to CMI. Growth hormone response to CMI challenge predicts treatment response (> or = 25% decreases YBOCS from baseline) to oral CMI at 8 weeks.RESULTSIn response to CMI challenge, OCD patients exhibit blunted cortisol and exaggerated growth hormone response relative to normal controls. OCD patients differ from controls in "sadness" ratings, with control exhibiting increased dysphoria in response to CMI. Growth hormone response to CMI challenge predicts treatment response (> or = 25% decreases YBOCS from baseline) to oral CMI at 8 weeks.Growth hormone abnormalities associated with OCD in response to CMI challenge differentiates nonresponders after 8 weeks of oral CMI treatment from responders.CONCLUSIONSGrowth hormone abnormalities associated with OCD in response to CMI challenge differentiates nonresponders after 8 weeks of oral CMI treatment from responders. |
Author | Carson, Stanley W Sallee, Floyd R Sethuraman, Gopalan Koran, Lorrin M Pallanti, Stefano |
Author_xml | – sequence: 1 givenname: Floyd R surname: Sallee fullname: Sallee, Floyd R organization: Department of Psychiatry and Behavioral Sciences, Medical University of South Carolina, Charleston, South Carolina, USA – sequence: 2 givenname: Lorrin M surname: Koran fullname: Koran, Lorrin M organization: Department of Psychiatry and Behavioral Sciences, Stanford University Medical Center, Stanford, California, USA – sequence: 3 givenname: Stefano surname: Pallanti fullname: Pallanti, Stefano organization: Istituto di Neuroscienze, Florence, Italy – sequence: 4 givenname: Stanley W surname: Carson fullname: Carson, Stanley W organization: School of Pharmacy, University of North Carolina, Chapel Hill, North Carolina, USA – sequence: 5 givenname: Gopalan surname: Sethuraman fullname: Sethuraman, Gopalan organization: Department of Psychiatry and Behavioral Sciences, Medical University of South Carolina, Charleston, South Carolina, USA |
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Keywords | Clomipramine OCD intravenous Human Obsessive compulsive disorder Intravenous administration Serotonin Psychotropic Treatment efficiency Anxiety disorder Prediction Tricyclic compound Neurotransmitter Antidepressant agent Pretreatment |
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Snippet | Background: Challenge with intravenous clomipramine (CMI) is serotonin selective and has been reported to transiently exacerbate symptoms in... Challenge with intravenous clomipramine (CMI) is serotonin selective and has been reported to transiently exacerbate symptoms in obsessive-compulsive disorder... |
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SubjectTerms | Administration, Oral Adolescent Adult Affect - drug effects Biological and medical sciences Clomipramine Clomipramine - administration & dosage Double-Blind Method Drug Administration Schedule Female Human Growth Hormone - blood Humans Hydrocortisone - blood Infusions, Intravenous intravenous Male Medical sciences Neuropharmacology Obsessive-Compulsive Disorder - diagnosis Obsessive-Compulsive Disorder - drug therapy OCD Pharmacology. Drug treatments Psychoanaleptics: cns stimulant, antidepressant agent, nootropic agent, mood stabilizer..., (alzheimer disease) Psychology. Psychoanalysis. Psychiatry Psychopharmacology Serotonin Uptake Inhibitors - administration & dosage Treatment Outcome |
Title | Intravenous clomipramine challenge in obsessive-compulsive disorder: predicting response to oral therapy at eight weeks |
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