1.
Phase I/II multicenter ketogenic diet study for adult superrefractory status epilepticus.
Cervenka, MC, Hocker, S, Koenig, M, Bar, B, Henry-Barron, B, Kossoff, EH, Hartman, AL, Probasco, JC, Benavides, DR, Venkatesan, A, et al
Neurology. 2017;88(10):938-943
-
-
-
Free full text
-
Plain language summary
Superrefractory status epilepticus (SRSE) is a neurologic emergency that persists despite anti-seizure medication. The ketogenic diet (KD) has been shown to be successful for treating epilepsy and recent retrospective studies suggest KD may be effective for treating SRSE. The aim of this clinical trial was to investigate the feasibility, safety and efficacy of a ketogenic diet on SRSE in adults. After screening, this prospective multi-centre study enrolled 15 participants with SRSE. Participants received a classic ketogenic diet via gastronomy tube. Of the 14 participants whom completed KD treatment SRSE resolved in 11 participants. Five patients ultimately died. This study found KD is feasible in adults with SRSE, and further randomised controlled trials are required to establish comparative safety and efficacy.
Abstract
OBJECTIVE To investigate the feasibility, safety, and efficacy of a ketogenic diet (KD) for superrefractory status epilepticus (SRSE) in adults. METHODS We performed a prospective multicenter study of patients 18 to 80 years of age with SRSE treated with a KD treatment algorithm. The primary outcome measure was significant urine and serum ketone body production as a biomarker of feasibility. Secondary measures included resolution of SRSE, disposition at discharge, KD-related side effects, and long-term outcomes. RESULTS Twenty-four adults were screened for participation at 5 medical centers, and 15 were enrolled and treated with a classic KD via gastrostomy tube for SRSE. Median age was 47 years (interquartile range [IQR] 30 years), and 5 (33%) were male. Median number of antiseizure drugs used before KD was 8 (IQR 7), and median duration of SRSE before KD initiation was 10 days (IQR 7 days). KD treatment delays resulted from intravenous propofol use, ileus, and initial care received at a nonparticipating center. All patients achieved ketosis in a median of 2 days (IQR 1 day) on KD. Fourteen patients completed KD treatment, and SRSE resolved in 11 (79%; 73% of all patients enrolled). Side effects included metabolic acidosis, hyperlipidemia, constipation, hypoglycemia, hyponatremia, and weight loss. Five patients (33%) ultimately died. CONCLUSIONS KD is feasible in adults with SRSE and may be safe and effective. Comparative safety and efficacy must be established with randomized placebo-controlled trials. CLASSIFICATION OF EVIDENCE This study provides Class IV evidence that in adults with SRSE, a KD is effective in inducing ketosis.
2.
A phase I trial of mushroom powder in patients with biochemically recurrent prostate cancer: Roles of cytokines and myeloid-derived suppressor cells for Agaricus bisporus-induced prostate-specific antigen responses.
Twardowski, P, Kanaya, N, Frankel, P, Synold, T, Ruel, C, Pal, SK, Junqueira, M, Prajapati, M, Moore, T, Tryon, P, et al
Cancer. 2015;121(17):2942-50
-
-
-
Free full text
-
Plain language summary
Prostate specific antigen (PSA) is a protein produced both by normal cells in the prostate and by prostate cancer cells. For men who have had prostate cancer, monitoring PSA levels can provide an early indication of recurrence of the disease. Naturally-occurring plant compounds, known as phytochemicals, may play a role in prostate cancer prevention, risk of recurrence, and therapy. This phase 1 trial evaluated the effects of white button mushroom (WBM) powder on PSA levels and determined the tolerability and biological activity of WBM. The 36 patients enrolled in this trial had previously undergone surgery and/or radiation treatment for prostate cancer and subsequently were found to have a continuously rising PSA level. Patients were given tablets containing WBM powder at doses from 4g to 14g (equivalent to 40g to 140g of fresh WBM). The mean reduction in PSA levels was 11%. Two patients receiving 8 and 14 g/d demonstrated complete response: their PSA declined to undetectable levels that continued for 49 and 30 months. Two patients who received 8 and 12 g/d experienced partial response: a decline of at least 50% in PSA levels. After 3 months of therapy, 13 (36%) patients experienced some PSA decrease below baseline. PSA levels remained stable in 5 patients. Patients who responded had higher levels of a cytokine called interleukin-15 (IL-15) at the beginning of this study, and experienced a decline in immuno-suppressive myeloid-derived suppressor cells (MDSCs) during the study. When comparing responders to non-responders, the following factors did not seem to affect the response: the daily mushroom dose, grade of cancer, baseline PSA level, weight, age, baseline testosterone levels and type of prior therapy. WBM powder therapy did not influence the levels of circulating androgen hormones: testosterone, dihydrotestosterone (DHT) and dehydroepiandrosterone (DHEA). The authors concluded that therapy with WBM appears to impact PSA levels and decrease immunosuppressive factors. Future trials should contain a placebo group and more research is needed to isolate the compound(s) from the WBM with anti-prostate cancer activity.
Abstract
BACKGROUND Each year in the United States, nearly 50,000 prostate cancer patients exhibit a rise in prostate-specific antigen (PSA) levels, which can indicate disease recurrence. For patients with biochemically recurrent prostate cancer, we evaluated the effects of white button mushroom (WBM) powder on serum PSA levels and determined the tolerability and biological activity of WBM. METHODS Patients with continuously rising PSA levels were enrolled in the study. Dose escalation was conducted in cohorts of 6; this ensured that no more than 1 patient per cohort experienced dose-limiting toxicity (DLT). The primary objective was to evaluate treatment feasibility and associated toxicity. The secondary objectives were to determine WBM's effect on serum PSA/androgen levels; myeloid-derived suppressor cells (MDSCs); and cytokine levels. RESULTS Thirty-six patients were treated; no DLTs were encountered. The overall PSA response rate was 11%. Two patients receiving 8 and 14 g/d demonstrated complete response (CR): their PSA declined to undetectable levels that continued for 49 and 30 months. Two patients who received 8 and 12 g/d experienced partial response (PR). After 3 months of therapy, 13 (36%) patients experienced some PSA decrease below baseline. Patients with CR and PR demonstrated higher levels of baseline interleukin-15 than nonresponders; for this group, we observed therapy-associated declines in MDSCs. CONCLUSIONS Therapy with WBM appears to both impact PSA levels and modulate the biology of biochemically recurrent prostate cancer by decreasing immunosuppressive factors.