Green tea extract improves cognition in Down Syndrome subjects

Published: 28-Jul-2016

Nutraceutical plus cognitive training improves some measures of cognition and behaviour in subjects with Down syndrome


New research published in Lancet Neurology and reported by CNN has found using a green tea extract (decaffeinated) in combination with cognitive training improves some measures of cognition and behaviour in subjects with Down syndrome.

Eighty seven volunteers aged 16 to 34 with Down syndrome were enrolled in the Phase II, randomised, controlled trial. The study was conducted at the IMIM-Hospital del Mar Medical Research Institute in Barcelona, Spain.

Participants were randomly assigned to take the decaffeinated green tea extract or a placebo for one year. All subjects also underwent cognitive training during the 12-month trial.

After one year of treatment, functional brain scans (fMRI) showed that epigallocatechin-3-gallate (EGCG)-treated subjects had improved neuronal connectivity in certain brain regions. Participants who took the green tea extract also scored significantly better on assessments of visual recognition memory, inhibitory control and adaptive behaviour compared with those who took the placebo.

'It's an important trial,' says Dr Steven Hirsh, Director of Clinical Research for Life Extension. 'The findings are very noteworthy and support further study in randomised controlled trials with larger sample sizes and durations. It is very encouraging that this catechin, EGCG, from green tea extract, has the potential to benefit people with Down syndrome.'

Down syndrome is a genetic condition that affects about 250,000 Americans. Individuals with Down syndrome have an extra full or partial copy of chromosome 21.

The team of researchers, led by Dr Rafael de la Torre, Programme Director of IMIM Hospital del Mar Medical Research Institute and study co-principal investigator, and Dr Mara Dierssen, Group Leader at Center for Genomic Regulation, Barcelona, Spain, and study co-principal investigator, proposed that EGCG might have conferred these benefits by inhibiting an enzyme called DYRK1A, which has been implicated in Down syndrome and neurodegenerative conditions including Alzheimer disease.

The level of DYRK1A-positive cells is elevated in certain regions of Alzheimer disease patients' brains, and is roughly 20-fold higher in the frontal cortex, compared with normal brains. DYRK1A is implicated in the formation of neurofibrillary tangles (via tau hyperphosphorylation) and amyloid plaques, both of which are features of Alzheimer disease.

Tea catechins may also modulate the damaging effects of amyloid-beta. Several animal studies have found that EGCG and related compounds from tea suppress amyloid-beta-induced cognitive dysfunction and neurotoxicity. Other possible mechanisms by which EGCG may influence cognition include epigenetic regulation, restoration of mitochondrial function and antioxidative functions.

In an earlier pilot study supported by Life Extension, Drs de la Torre and Dierssen's team showed that 3 months of EGCG treatment improved symptoms in individuals with Down syndrome, and in mice with a Down-syndrome-like condition characterised by overexpression of DYRK1A.

'We are excited that the benefits observed in the early pilot and preclinical research extended to this larger trial,' says Luke G. Huber, ND, MBA, Vice President of Product Innovation and Scientific Development at Life Extension. 'This new research adds to the growing body of evidence that suggests compounds in green tea, such as EGCG, may support cognitive health.'

In acknowledging the novelty of their findings and calling for more research, the Spanish research team noted: 'This study is the first well-powered trial that shows improvement in adaptive behaviour (functional academics) and brain-related changes in young adults with Down's syndrome. However, more research is needed to clarify the nature of the beneficial association between the EGCG and cognitive training intervention (synergistic or additive).'

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