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Research criteria for the diagnosis of Alzheimer's disease: genetic risk factors, blood biomarkers and olfactory dysfunction

Published online by Cambridge University Press:  01 August 2008

Jonathan Foster ,
Hamid Sohrabi ,
Giuseppe Verdile  and
Ralph Martins
Jonathan Foster
Affiliation:
Alzheimer's and Ageing, Edith Cowan University, Joondalup, Western Australia Email: j.foster@ecu.edu.au Sir James McCusker Alzheimer's Disease Research Unit, Hollywood Private Hospital, Nedlands, Western Australia Centre of Excellence for Alzheimer's Disease Research and Care, Western Australia; CSIRO Australian Imaging, Biomarker and Lifestyle (AIBL) Flagship Study of Ageing, Australia Neurosciences Unit, Health Department of Western Australia, Mt. Claremont, Western Australia
Hamid Sohrabi
Affiliation:
Alzheimer's and Ageing, Edith Cowan University, Joondalup, Western Australia Email: j.foster@ecu.edu.au Sir James McCusker Alzheimer's Disease Research Unit, Hollywood Private Hospital, Nedlands, Western Australia Centre of Excellence for Alzheimer's Disease Research and Care, Western Australia; CSIRO Australian Imaging, Biomarker and Lifestyle (AIBL) Flagship Study of Ageing, Australia School of Psychiatry and Clinical Neurosciences, University of Western Australia, Crawley, Western Australia
Giuseppe Verdile
Affiliation:
Alzheimer's and Ageing, Edith Cowan University, Joondalup, Western Australia Email: j.foster@ecu.edu.au Sir James McCusker Alzheimer's Disease Research Unit, Hollywood Private Hospital, Nedlands, Western Australia Centre of Excellence for Alzheimer's Disease Research and Care, Western Australia; CSIRO Australian Imaging, Biomarker and Lifestyle (AIBL) Flagship Study of Ageing, Australia
Ralph Martins
Affiliation:
Alzheimer's and Ageing, Edith Cowan University, Joondalup, Western Australia Email: j.foster@ecu.edu.au Sir James McCusker Alzheimer's Disease Research Unit, Hollywood Private Hospital, Nedlands, Western Australia Centre of Excellence for Alzheimer's Disease Research and Care, Western Australia; CSIRO Australian Imaging, Biomarker and Lifestyle (AIBL) Flagship Study of Ageing, Australia
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Extract

We note with interest the recently proposed new diagnostic framework published in Lancet Neurology entitled “Research criteria for the diagnosis of Alzheimer's disease: revising the NINCDS-ADRDA criteria” by Dubois et al. (2007).

Type
Letters
Information
International Psychogeriatrics , Volume 20 , Issue 4 , August 2008 , pp. 853 - 855
Copyright
© International Psychogeriatric Association 2008

We note with interest the recently proposed new diagnostic framework published in Lancet Neurology entitled “Research criteria for the diagnosis of Alzheimer's disease: revising the NINCDS-ADRDA criteria” by Dubois et al. (Reference Dubois2007).

We are generally positively disposed towards this framework, especially with regard to its emphasis (in the context of the extant scientific literature) on the delineation of sensitive and specific biomarkers for the diagnosis of Alzheimer's disease (AD). As Norman Foster (Reference Foster2007) observes in his commentary piece in Lancet Neurology, “the NINCDS-ADRDA criteria are showing their age and risk losing their relevance” in the context of recent scientific evidence. However, there is a relative paucity of information provided by Dubois et al. (Reference Dubois2007) in their article pertaining to (a) genetic risk factors and blood biomarkers for AD, and (b) the role of olfactory dysfunction as a potential predictor of AD.

With respect to (a), there is now accumulating evidence in support of APOE ε4 carriers (who represent half of all AD cases) being characterized by a different etiology from non-ε4 carriers (Snowden et al., Reference Snowden2007). An APOE ε4 gene-dosage effect is also present in AD, in which the risk increases from 20% when no ε4 alleles are present, to 90% when two copies are present. Therefore, the associations of the ε4 allele with AD should perhaps also be taken into consideration together with other factors when formulating novel diagnostic criteria for AD. Moreover, there has been a recent suggestion that other genetic considerations are also relevant: several studies have reported an association of AD with polymorphic markers in SORL1 (e.g. Rogaeva et al., Reference Rogaeva2007). In addition, given their high penetrance and causal relationships, genetic mutations associated with early onset AD (located on chromosomes 1, 14, and 21) should perhaps be considered separately when assessing individuals where there is a strong family history of AD (St George-Hyslop, Reference St George-Hyslop1998).

Blood biomarkers must also be considered given recent findings by Ray and colleagues (Reference Ray2007). These authors found that certain plasma proteins which have cell signaling functions can be used to classify AD and controls with up to 90% accuracy. The authors also suggest that analysis of these proteins from patients with mild cognitive impairment (MCI; i.e. pre-symptomatic AD) can be used to identify patients who are at risk of progressing further and developing AD. This article and other findings indicating that plasma levels of β amyloid are associated with increased risk of AD suggest that blood markers (perhaps together with genetic and cerebrospinal fluid markers) should be investigated as potential diagnostic biomarkers for AD.

Furthermore, while Dubois et al. have suggested that sensory deficits should be considered as relevant exclusion criteria for AD, we would like to challenge this proposal, specifically with respect to (b), the role of olfactory dysfunction as a potential predictor of AD (Burns, Reference Burns2000). In general terms, AD is characterized by an advancing wave of cortical atrophy that moves from limbic and temporal cortices into higher-order association and ultimately primary sensory motor areas. However, there is an exception to this general framework. Specifically, there is increasing evidence that the sensory olfactory cortex is implicated early in the progression of AD (Mesholam et al., Reference Mesholam1998). Evidence for the involvement of the olfactory system is threefold: (i) smell dysfunction has been noted in AD patients, APOE ε4 carriers and family members of AD patients; (ii) MCI patients and healthy subjects showing cognitive decline indicative of early stage AD manifest olfactory problems; and (iii) there is post-mortem evidence of neurofibrillary tangles and β-amyloid plaques located in the olfactory system of early AD patients. Given the burgeoning literature regarding the involvement of the olfactory system in very early stage/prodromal/preclinical AD (see Hawkes, Reference Hawkes2006; Wilson et al., Reference Wilson2007), we propose that serious consideration should be given to the proposal that olfactory dysfunction should also be incorporated into a revised framework for the reliable diagnosis of AD (Burns, Reference Burns2000).

In addition, specific diagnostic criteria pertaining to the potentially important dichotomy between familial (early onset) versus sporadic (late onset) AD – and the possible relevance of age at the time of diagnosis – are not clearly addressed by Dubois et al.

A further comment concerns the characterization of the precursor state to full-blown AD. While the authors question the use of the term “mild cognitive impairment” because of its potential ambiguity, we believe that the use of the terms “preclinical” and “prodromal” is not clearly operationalized by Dubois et al. The use of these terms in the manner proposed by the authors could therefore contribute towards further confusion, rather than clarifying the stages preceding AD.

References

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