Late Infantile Neuronal Ceroid Lipofuscinosis (LINCL)

1. Late Infantile Neuronal Ceroid Lipofuscinosis (LINCL) • Rare, autosomal recessive, fatal lysosomal storage disease with extensive CNS neurodegeneration • Caused by mutations in the CLN2 gene, coding for a tripeptidyl peptidase (TPP-I) that normally functions to remove waste membrane proteins • Prior studies have demonstrated high level, long term TPP-I expression in the brain following intracranial gene transfer using an AAV2-based vector expressing the human CLN2 cDNA (AAV2CUhCLN2)1 • AAV2 mediated gene transfer to the CNS corrects the storage defect in CLN2 knockout mice2 1 Sondhi et al, ASGT Abstract #6602 Passini et al. ASGT Abstract #427

2. Clinical Assessment of LINCL Challenge • To develop a non-invasive strategy to assess the efficacy of direct CNS administration of AAV2CUhCLN2 in clinical studies Strategy • Assess magnetic resonance spectroscopy as a method to evaluate the status of the CNS in children with LINCL over time

3. Demographic Characteristics of Study Population 1 MRS = magnetic resonance spectroscopy; nd = not done 2 LINCL rating scale based on Steinfeld et al, Am J Med Gen (2002); 112: 347-354

4. Magnetic Resonance Scan of Severe LINCL 1 2 Slice 1 Slice 2 Slice 3 Slice 4 4 3

5. Metabolite Levels in Voxels from Parenchyma and Ventricles Determined by Magnetic Resonance Spectroscopy of Subject with Severe LINCL CHO NAA CR LAC CHO = choline CR = creatine NAA = N-acetylaspartate LAC = lactic acid

6. Definition of Area in Cortex for Assessment by Magnetic Resonance Spectroscopy • Metabolite concentrations assessed in voxels indicated in slice 2

7. Examples of Metabolites in the Cortex BD001 Age 8 BD009, Age 5 CR CR CHO NAA LAC CHO NAA LAC BD005, Age 13 BD002, Age 9

8. Metabolite Levels in the Cortex 1. nd – not determined

9. Spatial Variation of N-acetylaspartate Levels in Subject with Severe LINCL 8 6 Level of N-acetylaspartate 4 2 0 Caudal / rostral Lateral • Due to substantial spatial variation, comparison of two MRS scans for the same subject requires careful alignment of the images

10. Age-dependence of Creatine and Lactate Levels in Cortex Subject 5 1 10 2 6 11 3 12 7 4 9 20 10 8 y = 8.9 - 0.53x r2 = 0.48 15 y = -5.1 + 1.2x r2 = 0.49 6 Creatine Lactate 10 4 5 2 0 0 0 2 4 6 8 10 12 14 0 2 4 6 8 10 12 14 Age (yr)

11. Age-dependence of Choline and N-acetylaspartate Levels in Cortex Subject 5 1 10 2 6 11 3 12 7 4 9 14 14 12 12 y = 12.7-0.74x r2 = 0.56 y = 13.6 - 0.90x r2 = 0.62 10 10 8 8 Choline N-acetylaspartate 6 6 4 4 2 2 0 0 0 2 4 6 8 10 12 14 0 2 4 6 8 10 12 14 Age (yr)

12. Reproducibility of N-acetylaspartate Level Between two MRS Scans of the Same Subject Left Right Left Right Local increase Subject #3 Subject #1 Local decrease 6.0 6.0 3.0 3.0 0.0 0.0 Change in NAA level (1st scan – 2nd scan) Change in NAA level (1st scan – 2nd scan) -3.0 -3.0 -6.0 -6.0 Caudal Rostral Caudal Rostral • Changes in N-acetylaspartate level are small and spatially uniform

13. Summary • Magnetic resonance spectroscopy scans of children with LINCL show age-dependent decreases in the levels of choline, creatine and N-acetylaspartate, and an age dependent increase in levels of lactate • N-acetylaspartate provides the most reliable parameter of age-dependent changes • Duplicate MRS on the same subject can be registered, demonstrating similar local metabolite levels • Assessment of local N-acetylaspartate levels in serial MRS scans following gene transfer have the potential to show areas of the brain that are spared from progression of the disease