Effect of Milnacipran on Pain in Fibromyalgia (Forest)

University of California San Diego

Status and phase

Completed

Phase 4

Conditions

Fibromyalgia

Treatments

Drug: Milnacipram

Study type

Interventional

Funder types

Other

Industry

Other U.S. Federal agency

Identifiers

NCT01288807

100686

Details and patient eligibility

About

The investigators want to study the effects of milnacipran treatment on neurotransmitter release in fibromyalgia.

Full description

Fibromyalgia (FM) is a chronic pain condition with significant morbidity. Current research suggests a primarily central mediation of the widespread pain including central sensitization at the spinal level and abnormal pain processing at the cerebral level. Findings in FM patients include abnormal neurotransmitter levels in cerebrospinal fluid (CSF), abnormal activation of cerebral pain processing areas and abnormal peripheral pain and sensory thresholds. Continuous low level spinal cord activation by primary nociceptive afferents (C and A delta fibers) is believed to significantly drive the central sensitization. One major spinal neurotransmitter released by these pain fibers is substance P (SP). Several studies have shown that FM patients have up to three times higher baseline SP levels in the CSF compared to controls. Since spinal neurotransmitter release and therefore nociceptive afferent activity is also regulated via a descending inhibitory pathway releasing norepinephrine (NE) and serotonin (5HT), decreased activity of this pain modulating system could also be involved in abnormal pain processing in FM. Indeed, there is support in the literature for decreased CSF levels of both NE and 5HT or their metabolites. Milnacipran, a NE and 5HT reuptake inhibitor, has been shown to potentially effectively reduce FM pain and symptoms of FM by affecting the above pathologies.

The investigators propose an open label clinical trial with milnacipran 200 mg over 12-weeks in order to investigate the pain pathway in FM patients at peripheral and spinal levels before and after treatment. In addition, the investigators will assess pain intensity and symptoms of FM before, during and after treatment. To determine if there are peripheral effects, the investigators will characterize the systemic neurotransmitter release and their metabolites in plasma. The investigators will also measure the heart rate variability using an electrocardiogram to look for effects on the sympathetic nervous system.

Enrollment

8 patients

Sex

Female

Ages

18+ years old

Volunteers

No Healthy Volunteers

Inclusion criteria

Female age 18 or older
Written informed consent and written release of health and research study information
Diagnosis of Fibromyalgia
Participant has pain greater than 4 on the NRS of 0 to 10 on average over the last week prior to initial evaluation that interferes with function most days per week
Pain duration greater than 6 months
Negative urine pregnancy test on experimental day 1 and 2 and on first day of treatment prior to administration of study medication and fluoroscopy
Ability to speak and understand English, to follow instructions, and fill out study questionnaires
Likely to complete all required visits
Must be ambulatory and able to lay prone for 30 minutes

Exclusion criteria

Any condition or situation that in the investigator's opinion may put the participant at significant risk, confound the study results, or interfere significantly with the participant's participation in the study
Serious, unstable medical illness that could lead to hospitalization over the next three months; and/or a DSM-IV diagnosis(es) with active problems within the last six months, such as: schizophrenia, bipolar disorder, antisocial personality disorder, or substance use disorder
Known, uncontrolled, serious systemic disease, including: hypertension and/or tachyarrythmia
Females who are pregnant, breast feeding, or who plan to become pregnant, or who may potentially become pregnant
Allergy or sensitivity to any component of the study medication or to contrast dye
Patients on coumadin, heparin, or any other known increase risk of bleeding
Signs of increased intracranial pressure
Patients who are unable to continue current pain medication
Allergy or contraindication to acetaminophen
Use of monoamine oxidase inhibitors
Uncontrolled narrow-angle glaucoma