34 Thus, the NMDA antagonist PPI model docs not appear to be another instance of receptor tautology and may, therefore, provide a pathway to identification of novel molecular targets for treatments of schizophrenia. PPI in the post-MATRICS era By virtue of the MATRICS program, the new focus of drug discovery in Quisinostat datasheet schizophrenia is on the identification
of potential procognitive cotreatments. In contrast, the work discussed above addressed the effects of antipsychotic treatments on PPI in animal models. In the post-MATRICS era, the question arises as to the possible utility of PPI models in the discovery process for procognitive cotreatments. The previous work in rodents indicated that the dopamine PPI model is reliably predictive Inhibitors,research,lifescience,medical Inhibitors,research,lifescience,medical of existing antipsychotics, while
the NMDA PPI model is insensitive to first-generation antipsychotics, but responsive to clozapine and some other second-generation compounds. Since the anticipated application is for cotreatments to be used in patients already stably treated with antipsychotic drugs, any animal model that is responsive to first-generation antipsychotics is likely to be uninformative. Given that the patients will already be treated with antipsychotics having antagonist actions at dopamine D2 receptors, dopamine agonist models are inappropriate. In Inhibitors,research,lifescience,medical contrast, the PPI models based on the effects of NMDA antagonists may be of considerable value in this context. Antipsychotic effects on PPI and cognition in patients The fundamental difficulty in evaluating
the potential applicability of any animal model for the Inhibitors,research,lifescience,medical prediction of procognitive agents in schizophrenia is the absence of any established positive control compound. That is, in the absence of any path to registration of procognitive treatments that do not also treat positive symptoms of schizophrenia, virtually no studies have been done in this specific area. What we do have some information about, however, arc comparisons of different classes of antipsychotic drugs on both cognition and PPI in patients with schizophrenia. As summarized recently by Hagan and Jones,35 it is clear Inhibitors,research,lifescience,medical that first-generation antipsychotics, which are principally dopamine D2 antagonists, have no beneficial effects on cognition. Similarly, as evident from the many early demonstrations of deficient PPI in antipsychotic-treated patients, first-generation compounds do not normalize PPI in schizophrenia.21,36 With respect to second-generation antipsychotics, and in particular ALOX15 clozapine, the evidence is less clear, but indicates that clozapine and some other multireceptor antagonist antipsychotics may have some salutary influences on cognition37 and appear to be associated with relatively normal PPI.36 Of particular interest in this regard is a crosssectional study indicating that clozapine treatment, relative to typical antipsychotic treatments, is associated with reduced PPI deficits in patients with schizophrenia.