Investigating the Ketogenic Diet As Treatment for Primary Aggressive Brain Cancer: Challenges and Lessons Learned

Schwartz, Kenneth A.; Noel, Mary; Nikolai, Michele; Chang, Howard T.

doi:10.3389/fnut.2018.00011

Cited by 43 publications

(37 citation statements)

References 38 publications

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“…While preclinical data suggests great promise for KD treatment of GBM, few clinical studies have been done [24][25][26][27][28][29][30][31]. Part of the reason is the difficulty of doing KD.…”

Section: Feasibilitymentioning

confidence: 99%

“…KD poses three main challenges: lack of palatability, the complicated nature of meal preparation, and lack of standardization. Of the four published KD GBM studies with > 2 patients, three concluded that KD cannot be tolerated for more than 6-12 weeks [26][27][28], and that the maximally tolerated diet is 3:1 with 20 g CH. In a German study of restrictive calorie ketogenic diet in end-stage malignant tumors only 5/16 subjects completed the 3-month treatment period [32].…”

Section: Feasibilitymentioning

confidence: 99%

“…In patients with GBM, hyperglycemia is associated with shorter survival [23]. There have been seven reports of KD treatment of patients with GBM: 3 of 1-2 patients and 4 with 9-20 patients [24][25][26][27][28][29][30].…”

Section: Introductionmentioning

confidence: 99%

“…These studies have varied widely. They have ranged in treatment duration from 6-14 weeks, in disease stage from adjunctive treatment with standard initial care to recurrent GBM, in diet design CH content from 60 g CH/day or 25% of calories derived from CH to 4:1 KD [26][27][28]30], in fat content, and in presence, absence and degree of caloric restriction.…”

Section: Introductionmentioning

confidence: 99%

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Treatment Of Glioblastoma Multiforme With “classic” 4:1 Ketogenic Diet Total Meal Replacement

Klein

Tyrlíková

Zuccoli

et al. 2019

Preprint

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Background: Glioblastoma (GBM) has poor survival with standard treatment.Experimental data suggest potential for metabolic treatment with low carbohydrate ketogenic diet (KD).Few human studies of KD in GBM have been done,handicapped by difficulty and variability of the diet,compliance and feasibility issues.We have developed a novel KD approach of total meal replacement (TMR) program using standardized recipes with ready-made meals.This pilot study evaluated feasibility,safety,tolerability and efficacy of GBM treatment using TMR program with “classic” 4:1 KD. Methods: GBM patients were treated in an open-label study for 6 months with 4:1 [fat]:[protein + carbohydrate] ratio by weight,10 g CH/day,1600 kcal/day TMR.Patients were either newly diagnosed (group 1) and treated adjunctively to radiation and temozolomide,or had recurrent GBM (group 2).Patients checked blood glucose and blood and urine ketone levels twice daily and had regular MRIs.Primary outcome measures included retention,treatment-emergent adverse events (TEAEs) and TEAE-related discontinuation.Secondary outcome measures were survival time from treatment initiation and time to MRI progression. Results: Recruitment was slow,resulting in early termination of the study. Eight patients participated,4 in group 1 and 4 in group 2.Five (62.5%) subjects completed the 6 months of treatment,4/4 subjects in group 1 and 1/4 in group 2.Three subjects stopped KD early:2 (25%) because of GBM progression and one (12.5%) because of diet restrictiveness.Four subjects,all group 1,continued KD on their own, three until shortly before death,for total of 26, 19.3 and 7 months, one ongoing. The diet was well tolerated.TEAEs,all mild and transient,included weight loss and hunger (n=6) which resolved with caloric increase,nausea (n=2),dizziness (n=2),fatigue and constipation (n=1 each).No-one discontinued KD because of TEAEs. Seven patients died.For these, mean (range) survival time from diet initiation was 20 months for group 1 (range 9.5-27) and 12.8 months for group 2 (6.3-19.9). Mean survival time from diagnosis was 21.8 months for Group 1 (11-29.2) and 25.4 for group 2 (range 13.9-38.7). One patient with recurrent GBM and progression on bevacizumab experienced a remarkable symptom reversal,tumor shrinkage and edema resolution 6-8 weeks after KD initiation and survival for 20 months after starting KD. Conclusions: Treatment of GBM patients with 4:1 KD using total meal replacement program with standardized recipes is feasible and well tolerated.

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Section: Feasibilitymentioning

confidence: 99%

Section: Feasibilitymentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Treatment Of Glioblastoma Multiforme With “classic” 4:1 Ketogenic Diet Total Meal Replacement

Klein

Tyrlíková

Zuccoli

et al. 2019

Preprint

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“…Diet adherence and compliance remain significant barriers to successful implementation and an adequate assessment of KD efficacy. Common methodologies to assess and document KD adherence in adults beyond patient self-report include frequent measurements of serum β-hydroxybutyrate or urine acetoacetate concentrations during the first few weeks on the diet and/or collection of dietary food records [57,121,128]. As examples, daily urine ketone assessments are traditionally used in adults with epilepsy during MAD initiation until moderate to large levels of ketosis are reached and serum ketone assessments using drops of blood from a finger stick have been used to guide short-term KD therapy in patients with GBM [53,128].…”

Section: Management Of Adverse Effects and Poor Compliance In Adultsmentioning

confidence: 99%

Diet in Brain Health and Neurological Disorders: Risk Factors and Treatments

2019

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research focuses on the neuropsychology of memory and other cognitive disorders as they appear in Alzheimer's disease, Huntington's disease, and other dementia syndromes. He has also investigated the cognitive changes associated with epilepsy and its treatments, the psychological consequences of genetic testing for neuropsychiatric disorders, and improved methods for neuropsychological assessment. Dr. Brandt is a Fellow of both the American Psychological Association and the Association of Psychological Science, and is board-certified by the American Board of Clinical Neuropsychology. In 2015, he was bestowed the Distinguished Career Award by the International Neuropsychological Society. vii

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