PT  - JOURNAL ARTICLE
AU  - Giuseppe Esposito
AU  - Giampiero Giovacchini
AU  - Jeih-San Liow
AU  - Abesh K. Bhattacharjee
AU  - Dede Greenstein
AU  - Mark Schapiro
AU  - Mark Hallett
AU  - Peter Herscovitch
AU  - William C. Eckelman
AU  - Richard E. Carson
AU  - Stanley I. Rapoport
TI  - Imaging Neuroinflammation in Alzheimer&#039;s Disease with Radiolabeled Arachidonic Acid and PET
AID  - 10.2967/jnumed.107.049619
DP  - 2008 Sep 01
TA  - Journal of Nuclear Medicine
PG  - 1414--1421
VI  - 49
IP  - 9
4099  - http://jnm.snmjournals.org/content/49/9/1414.short
4100  - http://jnm.snmjournals.org/content/49/9/1414.full
SO  - J Nucl Med2008 Sep 01; 49
AB  - Incorporation coefficients (K*) of arachidonic acid (AA) in the brain are increased in a rat model of neuroinflammation, as are other markers of AA metabolism. Data also indicate that neuroinflammation contributes to Alzheimer&#039;s disease (AD). On the basis of these observations, K* for AA was hypothesized to be elevated in patients with AD. Methods: A total of 8 patients with AD with an average (±SD) Mini-Mental State Examination score of 14.7 ± 8.4 (mean age, 71.7 ± 11.2 y) and 9 controls with a normal Mini-Mental State Examination score (mean age, 68.7 ± 5.6 y) were studied. Each subject received a 15O-water PET scan of regional cerebral blood flow, followed after 15 min by a 1-11C-AA scan of regional K* for AA. Results: In the patients with AD, compared with control subjects, global gray matter K* for AA (corrected or uncorrected for the partial-volume error [PVE]) was significantly elevated, whereas only PVE-uncorrected global cerebral blood flow was reduced significantly (P &amp;lt; 0.05). A false-discovery-rate procedure indicated that PVE-corrected K* for AA was increased in 78 of 90 identified hemispheric gray matter regions. PVE-corrected regional cerebral blood flow, although decreased in 12 regions at P &amp;lt; 0.01 by an unpaired t test, did not survive the false-discovery-rate procedure. The surviving K* increments were widespread in the neocortex but were absent in caudate, pallidum, and thalamic regions. Conclusion: These preliminary results show that K* for AA is widely elevated in the AD brain, particularly in regions reported to have high densities of senile (neuritic) plaques with activated microglia. To the extent that the elevations represent upregulated AA metabolism associated with neuroinflammation, PET with 1-11C-AA could be used to examine neuroinflammation in patients with AD and other brain diseases.