Early Onset Alzheimer Disease Clinical Trial
Official title:
Multi-Center, Double-Blind, Placebo-Controlled, Monotherapy Study of Neptune Krill Oil (NKO™) in Early Stage Alzheimer's Disease
The purpose of this study is to evaluate the efficacy of NKO™ softgels in reducing decline of global cognitive function as measured by the Neuropsychological Test Battery (NTB), in patients diagnosed with early stage Alzheimer's disease when compared to fish oil and a placebo after 24 weeks of treatment.
Alzheimer's disease (AD) is an irreversible, progressive neurodegenerative disorder,
characterized by gradual cognitive deterioration, changes in behavior and personality. These
symptoms are related to neurochemical changes, neural death, and the breakdown of the
inter-neural connections. Loss of short-term memory is often the first sign, followed by
cognitive deficits involving multiple functions. Early stages of AD and mild cognitive
impairment are characterized as milder forms of memory loss or cognitive impairment that
could precede the onset of dementia and AD. Prevention of further cognitive decline
inpatients with these possible precursor conditions is of paramount importance given that
reversibility of AD is not possible.
It is estimated there are currently about 5.1 million people with Alzheimer's disease (AD)
in the United States (Alzheimer's Association, 2007) and this number is expected to reach
13.2 millions by 2050 (Hebert et al., 2003). Alzheimer's is ranked as the 7th leading cause
of death in the US for people of all ages and the 5th for people aged 65 or older (National
Center for Health Statistics, 2004). In Canada it is 280,000 people over 65 that are
estimated to have AD, and over 750,000 are expected to have the disease by 2031 (Alzheimer
Society of Canada, 2006). It is estimated to 10% of all North Americans over the age of 70
years have early stage AD or mild cognitive impairment.
Older age, low educational level and APOE ε4 allele are risk factors for AD (Lindsay et al.,
2002). Moreover, patients having the APOE ε4 allele show an earlier and faster cognitive
decline while having the ε2 allele is related to a slower decline. Homozygotous ε4 patients
show an even earlier and faster decline than heterozygotes (Martins et al., 2005).
While symptomatic treatments have been the focus of therapeutic investigations for AD,
recent research efforts target the toxic effect of amyloid beta (Aβ) peptides in order to
modify the underlying pathophysiology of the disease.
The presently approved treatments give only small clinical improvement and do not prevent
the progression of the disease, from mild cognitive impairment to dementia and death (Birks
et al., 2000; AD2000 Collaborative Group, 2004; Birks, 2006; Birks & Harvey, 2006; Loy &
Schneider, 2006).
Alzheimer's disease is characterized by two main pathological features of the brain:
intracellular neurofibrillary tangles formed by abnormal protein τ (tau); and extracellular
neuritic plaques formed by β-amyloid peptides (Aβ) (Kuo et al., 1996). The overproduction of
Aβ42 is genetically induced but environmental risk factors are required to get fully
symptomatic AD (Grant et al., 2002).
Among these risk factors, low docosahexaenoic acid (DHA) is one of the most important
dietary risk factor for AD (Morris et al., 2005). The reasons for the impact of DHA on
learning and memory and the association with AD are unclear but could result from its loss
in synapses (Montine et al., 2004), which are normally rich in DHA (Salem et al., 2001),
where it is particularly important for postsynaptic transmission and neuroprotection (Bazan,
2003). Studies in animal models have consistently showed that brain n-3 fatty acid content
is highly dependent on dietary intake and aging (Favrere et al., 2000; Youdim et al., 2000;
Calon & Cole, 2007).
Several animal studies, has shown that increased DHA intake has been found to increase
hippocampal acetycholine levels and its derivatives, neuroprotectin DI, which deceased cell
death (Aid et al, 2005; Lukiw et al., 2005). A study conducted on aged mice showed that DHA
intake improved memory performance (Lim et al. 2001). In another Alzheimer's disease mouse
model, reduction in dietary DHA showed loss of postsynaptic proteins associated with
increased oxidation, which was localized in the dendrites. However, when a group of
DHA-restricted mice where given DHA, they showed signs that the DHA intake protected them
against dendritic pathology, implying that DHA could be useful in preventing cognitive
impairment in Alzheimer's Disease (Calon et al., 2004).
Several epidemiological studies have shown a protective effect associated with increased
fish intake (a direct source of omega 3 fatty acids) against dementia and cognitive
impairment decline (Kalmijin et al. 1997, Barberger-Gateau et al. 2002; Morris et al 2003).
Recently, one large randomized double-blind placebo-controlled study found 1.6 g DHA and 0.7
EPA may be beneficial in reducing risk for AD (Freund-Levi et al, 2006). In addition, there
is mounting evidence that dietary supplementation with Omega 3 Fatty acids may be beneficial
in different psychiatric conditions such as mood behaviour, depression and dementia (Bourre
et al., 2005; Peet and Stokes, 2005; Stoll et al., 1999).
Krill is a very small crustacean which thrives in deep cold ocean waters where it forms an
important part of the life chain, providing nutrition for an array of marine mammals, birds
and fish. Neptune Krill oil (NKO) is a rich source of omega-3 and omega-9 fatty acids and
phospholipids, which carry and thus functionalize the omega-3 fatty acids (EPA/DHA)
attached. Phospholipids are important in protecting membranes from toxic injury and free
radical attack (Everson, I et al. 2000). NKO contains two main potent antioxidants; a
carotenoid (astaxanthin) and a flavonoid (novel due to its animal source). Astaxanthin has
been shown to have a stronger antioxidant activity than alpha-tocopherol, beta-carotene,
lycopene and lutein. Flavonoids, traditionally extracted from fruits, plants, vegetables or
algae have been studied for more than 60 years and their antioxidant activity is undoubted.
The hypothesis that NKO will be effective in AD is based on the high content of
phospholipids with DHA and of antioxidants that cross the blood - brain barrier as well as
essential brain nutrients. In addition, NKO has been proven to increase HDL-C that is
related to decreased plague formation which is related to decreased blood supply to the
brain, one of the factors causing AD progression. The aim of the current study is to
challenge this hypothesis in a randomized double blind study.
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Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator), Primary Purpose: Treatment
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