90 These and other studies suggest that p-tau is promising in distinguishing AD from frontotemporal dementia
(FTD), with sensitivity and specificity rates of 85% to 90%. 90,91 A combination of various p-tau subtypes did not provide improved results in distinguishing between the groups due to ceiling effects. P-tau may also be useful in distinguishing AD from idiopathic normal pressure hydrocephalus (iNPII). A study found similarly altered concentrations of t-tau and Aβ42 in both groups compared with controls, while p-taul81P was considerably higher in the AD group only.92 The sensitivity and specificity rates were Inhibitors,research,lifescience,medical higher than 85%. A Ponatinib order systematic review discusses what clinical benefit p-tau might offer. The high negative predictive Inhibitors,research,lifescience,medical value of p-tau of approximately 90% appears to be particularly significant. This means that normal values rule out the presence of AD with
almost 90% probability.93 In MCI subjects, high p-tau231P concentrations correlated with a decline in cognitive performance and conversion to AD.94 Similar results were established for ptaul81P.95 The three p-tau subtypes presented above were comparable in this respect.96 High p-tau231P Inhibitors,research,lifescience,medical concentrations at the initial examination also correlated with structural disease progression, measured as the rate of hippocampal atrophy in the course of the disease.97 A recent European multicenter trial on CSF p-tau231 in MCI subjects has shown that Inhibitors,research,lifescience,medical the results for p-tau in predicting AD in this risk group are indeed stable and consistent throughout multiple centers. In this study p-tau proved to be a powerful candidate predictor of AD in MCI subjects even in a very short mean selleck chemicals observation interval of only 1 to 2 years.98
This result is particularly promising regarding clinical use of p-tau by general practitioners or consultants in order to Inhibitors,research,lifescience,medical inform patients as early as possible. A Swedish 6-year study investigated the predictive value of the combined t-tau, Aβ42, and p-taul81P (defined as a ratio) for AD in a group of 137 MCI patients.99 AD was able to be predicted in the MCI subjects with a sensitivity of 95% and a specificity of approximately 85% , both with a combination of t-tau and Aβ42 and with a combination of t-tau and the ratio of Aβ42/p-tau181P.99This suggests that a useful combination of markers may optimize prediction in a more heterogenous MCI population over a longer observation period. The single assay methods have been modified by using the Luminex xMAP® Drug_discovery technology (Luminex Corp, Austin, TX) based on flow cytometry, which allows several parameters to be determined at the same time; the three biomarker candidates presented here can thus be measured at once using a relatively small volume of CSF. The first multicenter results are promising.100 Determination of these parameters is implemented both in the US and the European dementia networks. The first round-robin study is currently being conducted.