Oxaliplatin is a novel platinum compound with clinical activity against several solid tumors. It has been associated with sensory neuropathies and, rarely, a neuromyotonia-like hyperexcitability syndrome; a form of peripheral neuropathy manifested by tremor and twitching activity of muscles. We present a case of hyperexcitability syndrome developed during the treatment of stage III appendiceal adenocarcinoma with oxaliplatin-containing regimen and was successfully treated with Pregabalin.
Oxaliplatin, a platinum derivative, is an important component of the chemotherapy regimen used for both early and advanced stage colorectal malignancies. The main dose limiting toxicity of this agent is neurotoxicity. This adverse event has two distinct syndromes. Sensory neuropathy is correlated with long term administration of oxaliplatin [
A 53-year-old white female presented at the emergency department with right lower quadrant abdominal pain and vomiting. A CT scan of the abdomen and pelvis revealed enlarged appendix along with inflammatory changes around the appendix and ileus. Subsequently, appendectomy was performed, and the pathology study was consistent with moderately differentiated adenocarcinoma of the proximal half of the appendix, with penetration of the visceral peritoneum, margins were not involved with invasive carcinoma. Upon this finding, the patient underwent right hemicolectomy, and the surgical pathology study showed metastatic adenocarcinoma in 2 out of 19 mesenteric lymph nodes. She had PET/CT scan which was negative, and the patient was staged at T4, N1, M0 (stage IIIB). Patient was started on adjuvant chemotherapy with Oxaliplatin, Leucovorin and 5 Fluorouracil. At completion of the second cycle, she experienced diffuse and significant muscle spasms involving her upper and lower extremities, along with peri-oral tingling and numbness, she required hospitalization , her neurological exam revealed increased tone of her upper and lower extremities bilaterally, serum electrolytes were within normal range including serum potassium and magnesium. The patient was started on Pregabalin at a dosage of 50 mg three times daily, and significant improvement of her symptoms occurred within 48 hours, patient was discharged on Pregabalin at the same dose. Adjuvant chemotherapy using same regimen was restarted as outpatient, throughout her adjuvant therapy, she was kept on Pregabalin, and she received one gram of magnesium sulfate and one gram of calcium gluconate before and after each Oxaliplatin infusion. The patient was able to complete her treatment.
Oxaliplatin, a platinum derivative, is an antineoplastic agent indicated for both early and late stage colorectal cancers. Although it can cause multiple neurologic toxicities not limited to paresthesias, peripheral neuropathy and visual disturbances, special attention should be paid to a rare and clinically distinct feature known as neuromyotonia-like hyperexcitability syndrome, which warrants immediate management including, dose reduction or drug withdrawal depending on the severity of the symptoms. Clinically neuromyotonia is characterized by muscle stiffness, delayed muscle relaxation and twitching [
The patient discussed above developed this syndrome during her adjuvant chemotherapy with oxaliplatin, 5 fluorouracil and leucovorin for stage III appendiceal adenocarcinoma. A work up for autoimmune etiology yielded was negative and she had not taken any new medicines or herbal supplements.
While the exact mechanism of neuromyotonia in humans remains unknown, considerable emphasis is given to the persistent sodium channel activity or decreased potassium conductance as a cause of axonal hyperexcitability [
Gabapentin in doses of 200 to 600 mg daily has been used in the empirical treatment of neurotoxcity secondary to platinum drug. It also blocks the repetitive firing of neurons in vitro. Although it resulted in a partial or complete response in some patients, gabapentin failed to improve the acute neurosensory toxicity [
Pregabalin, an amino acid derivative of gamma-amino butyric acid has a similar pharmacological profile to gabapentin but has been shown in studies to provide equivalent efficacy to gabapentin at much lower doses given its higher bioavailability and pharmacokinetics, thus resulting in fewer dose-related adverse events. Its influences on the GABAergic neurotransmission, translates into analgesic and anxiolytic effects which led to its FDA approval for Diabetic neuropathy and post herpetic pain neuralgia [
We decided to treat our patient’s Oxaliplatin induced Hyperexcitability with Pregabalin 50 mg three times a day given its distinct advantages over gabapentin. She was able to finish her adjuvant chemotherapy course successfully without recurrence of this syndrome.
Oxaliplatin is an important component of the chemotherapy regimens used for the treatment of both early and late stage colorectal malignancies; it can cause both acute and chronic neurologic toxicities. Hyperexcitability syndrome is a rare complication of oxaliplatin therapy. It is characterized by cramps, myotonia, and muscle twitching. It warrants immediate drug withdrawal or drug reduction.