Cyclocreatine treatment improves cognition in mice with creatine transporter deficiency
Yuko Kurosawa, … , Stephen C. Benoit, Joseph F. Clark
Yuko Kurosawa, … , Stephen C. Benoit, Joseph F. Clark
Published July 2, 2012
Citation Information: J Clin Invest. 2012;122(8):2837-2846. https://doi.org/10.1172/JCI59373.
View: Text | PDF
Research Article Neuroscience

Cyclocreatine treatment improves cognition in mice with creatine transporter deficiency

Abstract

The second-largest cause of X-linked mental retardation is a deficiency in creatine transporter (CRT; encoded by SLC6A8), which leads to speech and language disorders with severe cognitive impairment. This syndrome, caused by the absence of creatine in the brain, is currently untreatable because CRT is required for creatine entry into brain cells. Here, we developed a brain-specific Slc6a8 knockout mouse (Slc6a8–/y) as an animal model of human CRT deficiency in order to explore potential therapies for this syndrome. The phenotype of the Slc6a8–/y mouse was comparable to that of human patients. We successfully treated the Slc6a8–/y mice with the creatine analog cyclocreatine. Brain cyclocreatine and cyclocreatine phosphate were detected after 9 weeks of cyclocreatine treatment in Slc6a8–/y mice, in contrast to the same mice treated with creatine or placebo. Cyclocreatine-treated Slc6a8–/y mice also exhibited a profound improvement in cognitive abilities, as seen with novel object recognition as well as spatial learning and memory tests. Thus, cyclocreatine appears promising as a potential therapy for CRT deficiency.

Authors

Yuko Kurosawa, Ton J. DeGrauw, Diana M. Lindquist, Victor M. Blanco, Gail J. Pyne-Geithman, Takiko Daikoku, James B. Chambers, Stephen C. Benoit, Joseph F. Clark

×

Figure 6

Improved object recognition memory in Slc6a8–/y mice after cyclocreatine treatment.

Options: View larger image (or click on image) Download as PowerPoint
Improved object recognition memory in Slc6a8–/y mice after cyclocreatine...
Novel object recognition tests were conducted 3 hours after familiarization in Slc6a8–/y (n = 7 [cyclocreatine]; 5 [creatine and placebo]) and Slc6a8fl/y (n = 5 per group) mice before and after 9 weeks of treatment. The discrimination index was calculated as the difference between new and familiar object exploration times divided by total time spent in object zones. Data are mean ± SEM. **P ≤ 0.01, ***P ≤ 0.001 vs. Slc6a8fl/y.