Diane Portman, MD∗Correspondence information about the author MD Diane Portman, Kristine A. Donovan, PhD, Margarita Bobonis, MD Department of Supportive Care Medicine, Moffitt Cancer Center, Tampa, Florida, USA
Stiff person syndrome (SPS) is a disorder characterized by fluctuating, progressive, and painful spasms of the limbs, trunk, and face. The condition is frequently associated with other diseases, including malignancies.
Case Description
Comment
As stress and anxiety worsen manifestations of PSPS, and associated anxiety and depressive mood are common and result in social disability, psychological assessment of PSPS is advised.
Study has shown that cognitive behavioral therapy decreases anxiety and improves rigidity and stiffness.
PSPS-related physical and psychological symptoms may respond favorably to early immunotherapy, treatment of the underlying cancer, and use of drugs that act on the GABAergic system (Table 1). However, management of the disorder is challenging and progression with compromise of quality of life is common. In their quest for relief, patients may seek alternative treatments. As U.S. state–sanctioned medical cannabis programs proliferate and include indications for cancer and neurologic conditions, cannabinoids are increasingly likely to be trialed by patients with paraneoplastic syndromes.
Medication | Dose/Day | Mechanism of Action |
---|---|---|
Benzodiazepines | GABA-A agonist | |
Diazepam | 5–100 mg (1–6 mg divided doses), individualized and increased gradually over time | |
Clonazepam | 5–100 mg (1–6 mg divided doses, individualized and increased gradually over time | |
Lorazepam | 6–60 mg in divided doses, individualized and increased gradually over time | |
Baclofen | 5–60 mg oral in divided doses
50–800 mcg/day intrathecal |
GABA-B agonist |
Anticonvulsants | GABAergic and other modes of action | |
Tiagabine | 4–12 mg in divided or single dosing | |
Levetiracetam | 2000 mg in divided doses | |
Gabapentin | 3600 mg in divided doses | |
Others | ||
Botulinum toxin | Neuromuscular level inhibition | |
Tizanidine | 4–36 mg in divided doses | Central alpha-2 adrenergic agonist with presynaptic inhibitory effect |
Dantrolene | 100–200 mg in four divided doses | Muscle relaxant |
Immunomodulator or suppressants | Dose | |
Rituximab | Weekly infusion for one month
Or two doses of 350–500/m2 at two-week interval Repeat dose for relapse |
Monoclonal antibody
Immune modulator |
Intravenous immunoglobulin | 2g/kg over two to five days | Immunomodulator |
Plasma exchange | Removal of circulating autoantibodies, immune complexes, cytokines, and other inflammatory mediators | |
Cannabinoids | Trials of cannabis derivatives individualized and increased gradually over time | Presumptive effects on immune system, neuroinflammation, and CNS neuroprotection via CB2 and CB1 activation |
Cannabinoids exert their effects via the endocannabinoid system, which includes the cannabinoid receptors CB1 and CB2. CB1 receptors located in the CNS are involved in memory processing, motor function, appetite, and sensory perception. CB2 receptors are expressed in immune cells and are ascribed a role in modulating immune responses. Cannabinoids may affect the pathogenic mechanisms and symptoms of other autoimmune neurologic conditions with painful spasms, such as multiple sclerosis, owing to their ability to suppress neuroinflammation and exert neuroprotective effects in the CNS via activation of CB1 and CB2. Cannabinoid effects on the immune system may also be involved.
Given the autoimmune hypothesis of etiology and symptom overlap (spasticity and rigidity) with other cannabis-responding conditions, cannabinoids may benefit PSPS.
Disclosures and Acknowledgments
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Key Message: This article describes a case of paraneoplastic stiff person syndrome and a novel treatment paradigm including medical cannabis. The outcomes suggest that state medical marijuana program-sanctioned THC/CBD products may provide relief for patients with refractory symptoms in this autoimmune neurologic condition. Further study is indicated.