Table 2.

Quality assessment of studies included in the meta-analysis

	Barnes et al. (2007b)	Du et al. (2004)	Fox et al. (2005)	Hashimoto et al. (2005)	Jack et al. (2004)	Jack et al. (2003)	Kaye et al. (2005)	Thompson et al. (2004)	Wang et al. (2003)
Study type	Case series with controls	Case series with controls	Trial	Case series	Case series with controls	Trial	Case series with controls	Case series with controls	Case series with controls
AD Diagnostic criteria (imaging used in criteria)	NINCDS–ADRDA	NINCDS–ADRDA (imaging used to exclude other neuropathol.)	NINCDS–ADRDA (imaging supporting AD)	NINCDS–ADRDA (MMSE >15)	NINCDS–ADRDA/DSM IIIR (general committee consensus)	Mild–moderate AD (>50 years old)	NINCDS–ADRDA (mixture of community and clinical cohorts)	NINCDS–ADRDA/DSM- IV	DAT = CDR of 0.5
AD exclusion criteria	Change in diagnosis at subsequent follow-up or post-mortem confirmation of a differing disease	Other neuropathol., head trauma, alcoholism, psychiatric illness, epilepsy, hypertension, diabetes, major heart disease	Significant other neurological diseases. Medications which affect cognition	Other neuropathol./mental disorders/congnitive-affecting treatments/focal brain lesions seen on MRI	Symptoms unrelated to AD, depression	Non-AD disorders, major and/or unstable conditions such as seizure, PD or tumour	Substance abuse, depression, Parkinson’s disease, depression blood test used to screen for exclusionary medical conditions^a	Substance abuse, depression, psychiatric illness/head injury	Other confounding neuropsychol. Genetic family history of AD
Specific white matter damage exclusion criteria	N/R	N/R	N/R	N/R	Stroke	Substantial cerebro-vascular disease	N/R	White matter lesions >3mm on T2 images	N/R
White matter lesion quantification	N/R	Volume of white matter intensities measured at baseline. Distribution similar between subject groups	N/R	N/R	N/R	N/R	N/R	N/R	N/R
APOE genotype (% E4)	N/R	N/R	AD = 54	AD-C = 54, AD T = 65	C = 10, slow = 55, fast = 56	N/R	C = 22, mild AD =59, moderate=71	N/R	N/R
Gender (% male)	C = 47, AD = 39	C = 44, AD = 40	AD = 40	AD-C = 19, AD-T = 22	C = 42, slow = 39, fast = 42	AD-C =40^b, AD-T = 41^b	C = 48, mild = 52, moderate = 71	C = 50, AD = 41	C = 46, AD = 61
Treatments	N/R	N/R	Donepezil 60%, galantamine 5%, rivastigmine 21%, HRT 21%, Vit E 32%	Donepezil (AD-T). AD-C, Both groups allowed Vit E, non-steroidal anti-inflammatory, ginko biloba, lecithin	N/R	N/R	N/R	N/R	N/R
Drop-out if RCT	N/A	N/A	15 due to no post-baseline scan	N/A	N/A	N/R	N/A	N/A	N/A
Assessment of controls	N/R	MRI excluding neuropathol.	N/A	N/A	Normal neurological exam, Community dwelling	N/A	Yearly assessment of neuropsychol., physical and medical exam	N/R	CDR 0.0
Exclusion criteria for controls	N/R	Clinical history of alcoholism, psychiatric illness, epilepsy, hypertension, diabetes, major heart disease or head trauma (Du et al., 2003)	N/A	N/A	No active neurological disorder, psychoactive medication	N/A	As for AD, plus diabetes mellitus, hypertension, angina, arrhythmia, seizure disorder, cancer, COPD or renal disease^a	Same as AD	Other neuropsychiatric disorders, genetic family history of AD
Magnet strength (Tesla)	1.5	1.5	1.5	1.5	1.5	0.5–1.5	1.5	2	1.5
Sites	N/R	1	17	1	N/R	38	1	1	1
Protocol (thickness (mm))	1.5	1.4	1.5–1.8	1.5	1.6	1.6	4 (detailed in Kaye et al., 1997)	N/R	1
Measurement method Number of raters	Manual 1	Semi-automated Checked by 1	Manual 3^a	Manual 1	Manual 1	Manual 1	Manual 3^a	Manual 1	Semi-automated Team of experts for template as in Haller et al. (1997), N/R for landmark placement
Registered scans or TIV corrected	Registered	N/R	Registered	N/R	Registered	Registered as referenced in Jack et al. (1998)	TIV corrected^a	Registered	N/R
Whole Hc measured?	No (small part of tail excluded)	No (small part of tail excluded) as in Hsu et al. (2002)	No (small part of tail excluded)	No (white matter excluded), Tail excluded	No (small part of tail excluded)	No (small part of tail excluded)	No (body of hippocampus only as in Kaye et al., 1997)	No (small part of tail excluded)	No (exclusion of white matter of alveus and fimbria some of tail excluded)
Reliability, inter-/intra-rater, same/different acquisitions, repeated × n, number subjects, volume/rate	N/R	ICC 0.94, intra-rater different acquisitions. Repeated × 2 (assumed), N = 9, volume	N/R	ICC 0.98, CV 2.8%^c, intra-rater, same acquisition. Repeated × 3, N = 10, volume	ICC 0.91, IQR of difference in rate: 2.3 × 10⁻³, intra-rater, same acquisition. Repeated × 2, N = 18, rate	CV 0.28%^c, intra-rater, different acquisitions. Repeated × 2, N= 10, volume	ICC 0.90, intra-rater, same acquisition. Repeated × 5, N= 5, volume	ICC 0.99 ICC 0.98, intra- and inter-rater, respectively. Same acquisition. Repeated × 2, N= 10, volume	ICC 0.93, intra-rater (assumed), different acquisitions. Repeated × 2, N= 8, volume
Blinding of raters to diagnosis	Yes	Visually checked blinded to diagnosis	Blinded to treatment group	Blinded to AD-C/AC-T	Yes	Blinded to treatment group	Yes^a	Yes	N/R
Blinding of raters to order of scans	Yes	N/R	Yes	Yes	Yes	Yes	Yes^a	Yes	N/R

Key: AD, Alzheimer’s disease; C, control; DAT, dementia of Alzheimer type, ICC, intra-class correlation coefficient, CV, coefficient of variation; AD-C, control group of AD patients; AD-T, treated AD patients; APC, annualised percentage change; N/A, not applicable; N/R, not reported; CDR, clinical dementia rating; MMSE, mini mental state examination; neuropathol., neuropathologies; neuropsychol., neuropsychologies, COPD, chronic obstructive pulmonary disease; slow, slowly progressing AD; fast, quickly progressing AD; mild, mild AD; moderate, moderate AD.

Conveyed by personal communication.

Based on a wider group.

CV quoted by Jack et al. (2003) is calculated as a median (range 0.02–0.70%). CV quoted by Hashimoto 2005 was quoted for left and right hippocampus separately (right = 2.84% and left = 2.78%). This was calculated as standard deviation/mean, where standard deviation indicated square root value of the arithmetic mean of 10 variance estimates.