Administrating Oxytocin to Treat Treatment Schizophrenia and Schizo-affective Patients (OXY-S-01)

Social disability is a hallmark of schizophrenia, and improving social functioning in schizophrenia should improve patients' overall functioning and quality of life. Oxytocin (Granholm, McQuaid et al.) is a nine amino-acid neuropeptide synthesized in the hypothalamus, has found to modulate social behaviors in mammals, including humans (Insel and Young 2001; Kosfeld, Heinrichs et al. 2005). Among its influences on human social behavior are increased trust (Kosfeld, Heinrichs et al. 2005), empathy (Hurlemann, Patin et al. 2010) and eye contact (Guastella, Mitchell et al. 2008).

Impaired social behaviors are a core domain of Autism Spectrum Disorders (ASD) (Modahl, Green et al. 1998; Bartz and Hollander 2008); studies have shown that social disabilities have been associated with OT dysfunction in ASD, and have been improved by administration of intranasal OT (Hollander, Bartz et al. 2007; Andari, Duhamel et al. 2010; Guastella, Einfeld et al. 2010).

Furthermore, epigenetic changes in the genes encoding for OT have been demonstrated in autism (Gregory, Connelly et al. 2009)

Impaired social functioning is a hallmark of schizophrenia; studies show that plasma levels of endogenous OT are lower in schizophrenia patients compared to controls, and patients with lower levels of plasma OT have more positive symptoms (Kéri , Kiss et al. 2009; Kיri, Kiss et al. 2009; Rubin, Carter et al. 2010). Moreover, a recent study demonstrated a significant genetic association between OT and Arginine Vasopressin, another peptide linked with social behavior, and schizophrenia (Teltsh, Kanyas-Sarner et al. 2011). Only two published studies have investigated the therapeutic potential of OT in schizophrenia; both administered OT in addition to anti-psychotic treatment. Feifel (Feifel, Macdonald et al. 2010) reported a decrease in positive symptoms after 3 weeks of treatment, and Pedersen (Pedersen, Gibson et al. 2011) reported an improvement in social cognition. There is ongoing research aiming to validate these findings.

Vasopressin is also a peptide with a putative effect on social interaction (Ebstein, Israel et al. 2009; Heinrichs, von Dawans et al. 2009). In this proposed study we will assay salivary levels both of OT and vasopressin.

In this proposed study we intend to administer OT in a placebo-controlled, double-blind design to patients with schizophrenia. In addition to assessing the effect of OT on the symptoms of schizophrenia, this proposal has four characteristics which we believe are unique, and we hope will enable a large step forward in understanding the role of OT in schizophrenia.

• Social functioning: will be assessed using previously validated techniques, by video-taping interviews with schizophrenia patients. The quality of the social interactions will then be assessed, by raters blinded to treatment status. The assessment will , specifically focus on the gaze to the experimenter's face, vocalization (patient's vocal output, positive/negative tone, and fluent speech) and affect, body tone, movements, and other non-verbal signs. This technique was developed in Prof. Feldman's lab, and has been show to accurately assess social interactions (Feldman, Masalha et al. 2001; Feldman and Klein 2003; Feldman and Eidelman 2009; Feldman 2010). This technique will enable meticulous quantification of the putative effects of OT on social functioning in schizophrenia.
• Data from preclinical models of traumatic brain injury (Feeney, Gonzalez et al. 1982) and clinical studies in stroke patients (Crisostomo, Duncan et al. 1988; Scheidtmann, Fries et al. 2001; Taub, Uswatte et al. 2002)] suggest that new learning develops faster, has increased magnitude and is longer lasting under a combined intervention of drug and practice relative to learning occurring under either intervention in isolation. Similar thoughts have been expressed regarding compounds which putatively enhance cognition, in that patients who receive compounds which enhance cognition should be treated with cognitive remediation at the same time. We propose to apply this concept to OT. In this proposal, patients will be treated with cognitive-behavioral therapy (socially oriented CBT) focused on social interactions, emphasizing eye contact, body language, empathy, etc. Socially oriented CBT will be administered three times/week during the time period immediately after OT administration, when OT is active. There will be a control CBT condition addressing medication compliance and vocational rehabilitation, without any social orientation, with somewhat analogous demand characteristics. We hypothesize that the combined effects of OT co-administered with socially oriented CBT will be synergistic, i.e. greater than the effect of either alone.
• The effects of epigenetic variation on the effects of OT treatment will be examined by assessing epigenetic status of subjects, and these will be correlated with response to treatment. We will examine the methylation status of two CpG sites (-934 and -924) in the OXTR promoter. The epigenetic evaluation would detect whether the exogenously administered OT changes OXTR genes, their expression or function on OT levels and behavior.
• Two previous studies have administered 40 international units (IU) X2/d= 80 IU/d (Feifel, Macdonald et al. 2010) or 24 IU X2/d= 48 IU/d (Pedersen, Gibson et al. 2011), with no adverse effects. Based on this data, we propose to administer 24 IU X3/d= 72 IU. This dose is lower than Feifel et al. and no adverse effects were seen. Therefore, we are sure that thus dose is safe.