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Structural MRI as a Biomarker of Disease Progression in AD
Department of Diagnostic Radiology and MRI Research Lab
Presented by Clifford Jack, M.D.at the November 18, 2002
Peripheral and Central Nervous System Drugs Advisory Committee Meeting
Indirect measures of disease can be valid biomarkers of progression
• provided a plausible biologic link exists between change in the marker and progression of the disease itself
• changes in the marker are empirically proven to track with independent measures of progression
Applicable MR Measurements
• Structural MRI (link=cell loss to atrophy)• MR Spectroscopy • Functional MRI • Proton Diffusion• Perfusion• Relaxometry• Magnetization Transfer• Amyloid Plaque Imaging
The Rate of Medial Temporal Lobe Atrophy in Typical Aging and Alzheimer’s Disease
Neurology 1998;51:993-999
Objectives
• To determine the annualized rates of volume change of the hippocampus and temporal horn in cognitively normal elderly control subjects and individually matched AD patients
• To test the hypothesis that these rates were different
Controls(n=24) Cases (n=24)Mean ± SD Mean ± SD
Age 81.04 ± 3.78 yrs 80.42 ± 4.02 yrs
Education 14.75 ± 2.51 yrs 13.21 ± 2.83 yrs
MMSE 28.79 ± 1.28 20.74 ± 4.60
DRS 137.38 ± 4.69 108.48 ± 14.35
Interval Between MRI 1.96 ± 0.75 yrs 1.89 ± 0.68 yrsStudies
Characterization Of Subjects
Annual Percent Volume Change
Controls (n=24) Cases (n-24) P-value* Mean SD Mean SD
Hippocampal -1.61.4 -4.01.9 <0.001Temporal Horn 6.27.69 14.28.5 0.002
*Rank sum test of difference between cases and controls
Conclusion
• Reasonable 1st step: expected differences in rates between AD and controls were observed, but it did not prove that changes in imaging tracked with changes in independent measures of disease progression
• Rates were approximately 2.5 times greater in AD than in individually age and gender matched control
Rates of Hippocampal Atrophy in Normal Aging, Mild Cognitive Impairment, and
Alzheimer's Disease
Neurology, 2000;55:484-489
Objective:Transition Analysis
• To test the hypothesis that change on imaging (rates of hippocampal atrophy) match clinical change
• Use clinical transition (or lack of) as gold standard independent measures of progression
Methods
• 129 subjects from the ADRC/ADPR who met established criteria for normal controls, mild cognitive impairment (MCI), or probable AD at entry
• Controls and MCI patients could either remain cognitively stable or could decline
• MRI at initial & FU clinical assessment
Age at 1st MMSE Duration between MRI baseline and followup
MRI in years
Normal-Stable 80.4 ± 6.4 28 ± 1.6 3.0 ± 0.5(N=48) (62, 97) (23, 30) (2.0, 3.9)
Normal-Decliner 82.3 ± 5.8 28 ± 1.7 3.3 ± 0.4 (N=10) (76, 95) (25, 30) (2.7, 4.0) MCI-Stable 77.9 ± 8.0 24 ± 1.9 2.9 ± 0.5(N=25) (60, 92) (23, 30) (2.1, 4.0)
MCI-Decliner 77.3 ± 8.0 24 ± 3.2 2.9 ± 0.6(N=18) (64, 94) (18, 30) (2.1, 3.9)
AD 73.8 ± 11.3 22 ± 4.3 2.9 ± 0.5(N=28) (51, 93) (14, 29) (2.1, 3.9)
Descriptive Information
PERCENT ANNUAL CHANGE IN HIPPOCAMPAL VOLUME BY
FOLLOWUP CLINICAL GROUP
Normal-Stable (N = 48) -1.7 ± 0.9
Normal-Decliner (N = 10) -2.8 ± 1.7
MCI-Stable (N = 25) -2.5 ± 1.5
MCI-Decliner (N = 18) -3.7 ± 1.5
AD (N = 28) -3.5 ± 1.8
Values in table represent mean ± SD (range)
Conclusion
• Rates of hippocampal atrophy match the change in cognitive status (or lack of) over time in elderly persons who lie along the cognitive continuum from normal to MCI to AD
• Validation of change in MRI volume as a biomarker of Dz progression
Rates of Atrophy by Technique and by Clinical Group
Objective
• Are some techniques better measures of progression than others at different disease stages?
• To compare the annualized rates of atrophy by technique among clinical groups (normal -stable, normal-converter, MCI -stable, MCI-converter, AD-slow progressor, and AD-fast progressor)
Structures Measured: Rates of Change
• Hippocampus• Entorhinal Cortex (ERC)• Whole Brain • Ventricle
Whole Brain Ventricle GROUP Ann% ch GMM GMM HF ERC
Normal Stable Mean -0.4-0.4 1.81.8 -1.5 -2.7 -1.5 -2.7
Normal Converter Mean -0.7-0.7 3.33.3 -3.1 -5.3 -3.1 -5.3
MCI Stable Mean -0.4-0.4 2.82.8 -1.8 -4.8 -1.8 -4.8
MCI Converter Mean -0.9-0.9 4.04.0 -4.0 -6.8 -4.0 -6.8
AD Slow Progressor Mean -1.3-1.3 4.24.2 -3.5 -7.2 -3.5 -7.2
AD Fast Progressor Mean -1.6-1.6 6.66.6 -5.2 -10.2 -5.2 -10.2SDSD 0.8 2.3 3.0 4.7
(Mean1-Mean2) Whole Brain Ventricle (SD1*SD1)+(SD2*SD2) GMM GMM HF ERC
Normal Stable vs. 0.37 0.92 0.88 0.83Normal Converter
MCI Stable vs 0.87 0.56 1.00 0.38MCI Converter
AD Slow Progressor vs 0.25 0.72 0.42 0.41AD Fast Progressor
Normal Stable vs 1.32 1.95 1.22 1.52AD Fast Progressor
Conclusions
• Structural MRI rates consistently follow expected correlations with clinical status and clinical transition = support for use as biomarker of Dz progression
• Appears to be some stage specific Dx sensitivity
Multi-Site Studies
• MilamileneMilamilene• ObjectiveObjective: To assess the technical
feasibility of using MRI measurements as a surrogate end point for disease progression in a therapeutic trial of Milamilene for AD
Methods
• 52 week controlled trial of Milameline, a muscarinic receptor agonist, N=450
• therapeutic trial itself was not completed • MRI arm of the study was continued • 192 subjects from 38 different centers
underwent 2 MRI with 1 yr interval • hippocampal and temporal horn volume
Annual Raw Annual % Percent Change Change Decliners (N=192) (N=192)
ADAS-Cog 4.1 16.4 65.1
MMSE -1.9 -8.4 65.1
GDS 0 0.0 38.5
Total Hippocampal mm3 -221 -4.9 99.0
Total Temporal Horn Volume mm3 616 16.1 85.4
Change from Baseline in Behavioral/Cognitive and MRI Variables
Power Calculations
• Per arm for 50% effect size (rate reduction Per arm for 50% effect size (rate reduction over 1 yr.)over 1 yr.)
• ADAS-Cog 320• MMSE 241• hippocampal volume 21• temporal horn volume 54
Conclusions
• Technical feasibility documented• Decline over time was more consistently
seen with imaging measures than behavioral/cognitive measures (p<0.001)
• Power calculations: sample sizes imaging<< behavioral/cognitive
Structural MRI as a Biomarker
In the absence of a positive therapeutic trial that incorporated
imaging, the best available evidence supporting the validity of MRI as a biomarker of progression would be multiple natural history studies that
consistently demonstrate concordant MRI and clinical changes
Acknowledgments
• R01 AG11378• R01 AG19142• AG16574 ADRC• AG06786 ADPR
Mayo ADRC and ADPR
Ronald C. Petersen, M.D., Ph.D. Dorla BurtonRuth H. Cha, M.S. Dianne FitchPeter C. O’Brien, Ph.D. Nancy HaukomSteven D. Edland, Ph.D. Kris JohnsonRobert Ivnik Ph.D. Martha MandarinoGlenn E. Smith, Ph.D. Joan McCormickBradly F. Boeve, M.D. Sheryl NessEric G. Tangalos, M.D. Kathy Wytaske David Knopman MD
MILAMILENE: Parke-Davis
M. Slomkowski, Pharm.D.S. Gracon, D.V.M.
T. M. Hoover, Ph.D.
MR LAB
Maria Shiung Kejal Kantarci Jeff Gunter Yuecheng XuMira SenkacovaKelly StewartMarina Davtian