Results

Individuals with SMI have a greater likelihood to be at risk for incapacity in making informed consent. Informed consent should be based on the clinical features of SMI and on evolving legal understandings of informed consent as an individual’s right, regardless of societal or health status. To hold the preconception that individuals with a certain psychiatric disorder do not have decision making capabilities violates their autonomy, re-enforces stigmatization, and unreasonably neglects the potential research contributions of this population. Several instruments can serve as tools to aid in determining capacity in research. Instruments vary by administration length, administrator training, and measurement

Results

In total, 273 psychiatrists and 245 PCPs completed the survey. Cumulative correct scores averaged 56% among psychiatrists and 45% among PCPs. Psychiatrists scored highest on questions regarding individualizing initial and ongoing treatments for patients with MDD (60% correct responses). PCPs scored highest on questions related to the ability to formulate treatment decisions based on use of scales to assess symptoms (50%). Significant gaps in both groups were observed related to the understanding of the theoretical basis of MDD and integrating this knowledge into treatment selection (44% vs 30%, average correct scores), appropriate use of patient-reported depression rating scales to discern disability or quality of life issues (42% vs 48%), appropriate use therapy in patients with comorbidities (44% vs 43%), and management of treatment-resistant depression (49% vs 33%). When participants were asked about the level of difficulty they encounter in selecting first-line antidepressant therapy based on mechanisms of action, the highest percentage in both specialties indicated difficulty on a level of 4 out of 7. Psychiatrists and PCPs who scored higher on assessment questions related to mechanism of action of antidepressants reported significantly less difficulty in selecting first-line therapies (P<0.05). Those who scored higher on the assessment felt more strongly that the content will impact their practice and that the number of planned practice changes corresponded to a higher number of barriers to better patient outcomes (P<0.05).

Results

For psychiatrists who participated in the CME activity, comparison of individually linked pre-assessment question responses to the respective post-assessment question responses demonstrates statistically significant improvements (N=304; P<.05). Correct responses on post-assessment questions were significantly higher after CME completion compared with the pre-assessment question responses, with an overall medium effect (d=0.493). While only 31 (10%) participants answered all 4 questions correctly on the pre-assessment, 95 (31%) answered them all correctly on the post-assessment. Between 10% and 33% of participants showed improvement in understanding individual learning concepts, and these concepts were reinforced for between 17% and 82% of learners. The biggest improvement was demonstrated in recognition of risk for antidepressant-induced switch to mania and recognition of side effects for established treatments; the need for further education was seen in awareness of side effects of investigational therapeutic agents.

Results

Patients who received GeneSight testing saved $1,035.60 on total medication costs annually vs. the TAU group. This was due to a mean increase from the pre- to post-testing period of $143.77 in medication costs per member per month (PMPM) in the TAU group (p<0.0001), compared to a mean increase of only $57.47 PMPM in the GeneSight group (p<0.0001). The resulting cost differential PMPM between the two groups was $86.30. Among those eligible for the secondary analysis, 24.8% of patients were placed in the ‘green’ category, 46.5% were placed in the ‘yellow’ category, and 28.7% were placed in the ‘red’ category. Patients stratified into the red category spent $2,050.12 more on medications over the 365 day period after GeneSight testing compared to those stratified into the green or yellow categories (p=0.0005), thus increasing the mean costs of the GeneSight group by $587.77.

Results

Data related to 685 patients was collected. Approximately 70% had a mood disorder and 29% had an anxiety disorder. Seventy three percent of patients were treatment resistant, having failed two or more treatment trials prior to genetic testing. Clinician-reported CGI-I data indicated that 87% of patients showed clinically measurable improvement post-Genecept. Strikingly, 91% of the treatment resistant patients also showed clinically measurable improvement. Patient reported data demonstrated significant increases in quality of life, as well as decreases in depression, anxiety, and medication side effects; response rates exceeded those reported in the seminal STAR*D trial at all levels.

Results

Children (N=280; mean age, 10.8 ą 3.0 years) diagnosed with ADHD (by Diagnostic and Statistical Manual of Mental Disorders, 4th Edition, Text Revision criteria) were screened and 230 entered the double-blind phase and were administered MPH-MLR 10 mg (n=49), MPH-MLR 15 mg (n=44), MPH-MLR 20 mg (n=45), MPH-MLR 40 mg (n=45), or placebo (n=47) and 221 completed the 1-week double blind phase. MPH-MLR resulted in significantly greater improvement versus placebo in mean ADHD-RS-IV score (P<0.05) and CGI-I score (P<0.05). Clinical significance was seen at each of the 4 MPH-MLR fixed doses. 200 subjects completed the subsequent 11-week open label phase, during which their MPH-MLR dose was optimized. There was continuing improvement in efficacy over time. QoL measures did not statistically improve during the one-week double-blind period but showed significant improvements by study end. The most common AEs were consistent with known MPH AEs. Most treatment-emergent AEs were mild or moderate in severity, and there were no serious drug-related AEs throughout the study.

Results

The evaluable population included 20 subjects. The least squares (LS) mean postdose SKAMP Total score was higher for placebo (2.18 vs. 1.32, P=0.0001) indicating greater improvement with treatment. No difference in SKAMP Total score between subjects who initially received MPH-MLR or placebo in the double-blind phase was noted. From hours 1-12, the mean of all LS SKAMP Total Scores was significantly better for MPH-MLR than placebo (P≤0.0261). No new or unexpected safety findings were noted in the study.

Results

The study population was 57% female with a mean age of 44.8 years and mean BMI of 37.5. A higher proportion of patients with OSA were in the group without use of Quetiapine (81%, n=17). Use of Quetiapine was not significantly associated with altered sleep efficiency, sleep latency, WASO, or the relative percentage of sleep stages. A notable, but not significant (p=0.08), increase in the REM latency was observed.

Results

In many cases, it was found that outcomes were improved when an NP was added to a physician’s practice. In fact, none of the studies evaluated in this review reported any negative outcomes when NPs were used as adjunctive or collaborative members of a team with a physician. No studies reported any declines in satisfaction with the addition of NPs. There were no studies that evaluated NP and physician collaboration in psychiatry.

Results

Lurasidone monotherapy resulted in significantly greater Week 6 improvement on the MADRS-6 score for the 20–60 mg and 80–120 dose groups vs placebo (−10.4 and −10.4 vs −6.9; P<0.001 for both comparisons). Onset of significant improvement in the MADRS-6 was observed at Week 1 for the higher dose group and at Week 2 for the lower dose group. In the more severe depression subgroup, lurasidone therapy (2 dosage groups combined vs placebo) was associated with significantly greater Week 6 improvement on the MADRS total score (−17.3 vs −11.8; P<0.001) and on the MADRS-6 (−11.7 vs −7.5; P<0.001). Week 6 effect size was greater for the severe (vs less severe) depression subgroup on the MADRS total score (0.56 vs 0.44), and the MADRS-6 score (0.62 vs 0.44). Treatment with adjunctive lurasidone, compared with placebo, was associated with significantly greater Week 6 improvement on the MADRS-6 score (−11.6 vs −9.1; P=0.003). Onset of significant improvement in the MADRS-6, for lurasidone compared with placebo, was observed at Week 3. In the severe depression subgroup, numerically greater Week 6 improvement was observed on the MADRS total (−17.5 vs −14.6; P=0.103) and MADRS-6 (−11.7 vs −9.7; P=0.091). The Week 6 effect size was smaller for the severe vs moderate group on the MADRS total score (0.25 vs 0.40) and the MADRS-6 score (0.25 vs 0.49).

Results

Monotherapy treatment with lurasidone was associated with significantly greater early sustained response (compared with placebo) for the 20-60 mg group (14.6% vs 3.9%; P=0.007) and the 80-120 mg group (11.3% vs 3.9%; P=0.036). Adjunctive lurasidone (with Li or VPA) was also associated with (non-significantly) greater early sustained response compared with placebo (18.9% vs 14.7%). In the monotherapy study, the majority of lurasidone responders at every week were also sustained responders; this was not the case for early placebo responders at Weeks 1, 2, and 3. The same study also saw a significantly greater proportion of remitters on lurasidone beginning at Week 4. In the adjunctive study, the majority of responders at each time point had sustained response to Week 6, regardless of treatment group; furthermore lurasidone + Li/VPA was associated with a significantly greater proportion of sustained responders (vs placebo + Li/VPA) from Week 3 onward. Adjunctive lurasidone treatment was also associated with a significantly greater proportion of remitters from Week 3.

Results

MADRS vs time profiles for lurasidone and placebo were adequately described using a linear dose-response relationship, built on an exponential asymptotic placebo model. A net improvement in MADRS due to lurasidone treatment (the drug effect) was significant (P<0.001) and a positive dose-response was detected. Age and use of concomitant medication had statistically significant covariate effects on placebo change. Overall, the dose-dependent effect of lurasidone indicates that higher doses are likely to produce greater improvement. The dose-response was consistent for both monotherapy and adjunctive therapy studies.

Results

At baseline, the prevalence of metabolic syndrome was similar in the adjunctive studies (lurasidone, 14.8%; placebo, 13.5%) and in the monotherapy study (lurasidone, 14.3%; placebo, 15.5%). After 6 weeks of adjunctive therapy, the prevalence of metabolic syndrome in the lurasidone vs. placebo groups was 17.0% vs. 12.4% (last observation carried forward; LOCF); after 6 weeks of monotherapy, the prevalence was 15.8% vs. 17.7% (LOCF). For patients who completed 6 months of extension phase treatment, the prevalence of metabolic syndrome was 23.8% (adjunctive therapy) and 17.9% (monotherapy). For the subgroup with metabolic syndrome at baseline in the adjunctive therapy studies (n=31), the following median changes were observed (completer analysis): weight (0.0 kg), cholesterol (−6.0 mg/dL), triglycerides (+11.0 mg/dL), and glucose (+2.0 mg/dL). For the subgroup with metabolic syndrome at baseline in the monotherapy study (n=30), the following median changes were observed: weight (−0.3 kg), cholesterol (−4.0 mg/dL), triglycerides (−22.0 mg/dL), and glucose (−2.0 mg/dL).

Results

At Week 6 endpoint, treatment with lurasidone (vs placebo) was associated with improvement vs placebo in the mean MADRS (−14.4 vs −11.9; P=0.003), CGI-BP-S (−1.7 vs −1.3; P=0.001), QIDS-SR16 (−7.4 vs −5.7; P<0.001), HAM-A score (−7.0 vs −5.0; P<0.001 [LOCF]), and Q-LES-Q (+18.5 vs +13.2; P<0.001). Responder rates (MADRS reduction ≥50%) were significantly higher with lurasidone vs placebo (48% vs 37%; P=0.002; LOCF-endpoint). Minimal LOCF-endpoint changes were observed for adjunctive lurasidone vs placebo in mean weight (+0.1 vs +0.2 kg), median total cholesterol (−4.0 vs −1.0 mg/dL), LDL (−3.0 vs −1.0 mg/dL), triglycerides (+4.0 vs −2.0 mg/dL), and glucose (0.0 vs 0.0 mg/dL). Discontinuation rates due to adverse events were similar for lurasidone vs placebo (5.8% vs 4.8%); adverse events (≥5% incidence) were nausea (13.9% vs 10.2%), Parkinsonism (12.8% vs 8.1%), somnolence (11.4% vs 5.1%), and akathisia (10.8% vs 4.8%).

Results

A total of 68% of patients completed the extension study. Adverse events (AEs; incidence ≥5%) for the monotherapy and adjunctive therapy groups, respectively, were 6.0% and 9.5% for akathisia, 11.1% and 5.6% for headache, 7.3% and 7.8% for nausea, 6.3% and 6.4% for insomnia, and 4.4% and 6.6% for anxiety; and 7.0% and 8.7% discontinued due to an AE. Mean changes in weight at Month 6, for the monotherapy and adjunctive therapy groups, respectively, were +0.45 kg and +0.90 kg; and median changes were 0.0 mg/dL and −1.5 mg/dL for total cholesterol, +6.0 mg/dL and +8.0 mg/dL for triglycerides, 0.0 mg/dL and +1.0 mg/dL for glucose, and +1.3 mg/dL and +1.3 mg/dL for prolactin. The incidence of treatment-emergent mania was 1.3% in the monotherapy treatment subgroup and 3.8% in the adjunctive subgroup. Mean changes in MADRS, from open-label baseline to month 6, was −6.9 in the monotherapy group and −6.5 in the adjunctive therapy group (OC analysis).

Results

In the combined lurasidone dose groups, the proportion of patients showing early improvement was similar for the PANSS ≥20% criterion and the CGI-S ≥1 criterion, respectively, at Week 1 (32.5% and 36.1%) and Week 2 (53.8% and 59.8%); but was lower at Week 3 for the PANSS ≥20% criterion (70.7% and 88.0%). Endpoint response in the lurasidone group was 50.2% using PANSS ≥40% responder criteria. For prediction of endpoint response (using the PANSS ≥40% criterion), PANSS ≥20% improvement at Week 1 had 46.6% sensitivity, 81.6% specificity, and AUCROC=0.660. CGI-S improvement ≥1 at Week 1 had 46.2% sensitivity, 74.0% specificity, and AUCROC =0.621. At Week 2, PANSS ≥20% improvement had 75.2% sensitivity, 67.8% specificity, and AUCROC =0.733. CGI-S improvement ≥1 at Week 2 had 74.4% sensitivity, 54.8% specificity, and AUCROC =0.650. At Week 3, PANSS ≥20% improvement had 91.9% sensitivity, 50.5% specificity, and AUCROC =0.730. At Week 3, CGI-S improvement ≥1 had 87.3% sensitivity, 43.7% specificity, and AUCROC =0.656.

Results

The LS mean (95% CI) treatment difference for change in BE days/week from baseline to week 11-12 significantly favored LDX (study 1: −1.35 [−1.70, −1.01]; study 2: −1.66 [−2.04, −1.28]; both P<0.001). Statistically significant improvements favoring LDX were seen for all key secondary endpoints (all P≤0.002) in both studies. In both studies, TEAEs reported by ≥10% of LDX participants were dry mouth, insomnia, and headache; mean pulse and blood pressure changes were consistent with known LDX effects.

Results

In the monotherapy study, treatment with lurasidone, in both daily dose ranges, was associated with significantly greater improvement in the MADRS (primary outcome) starting at week 2 through the week 6 endpoint. Significantly greater efficacy was also observed on secondary efficacy measures, including the Clinical Global Impression, Bipolar - Severity of Illness scale (CGI-BP-S), MADRS-6 (core items), Hamilton Anxiety Rating scale (HAM-A), and patient-rated measures of quality of life and functioning. In the first 6-week adjunctive therapy trial, treatment with lurasidone was associated with significantly greater improvement in the MADRS at week 3 through week 6 endpoint. Significantly greater efficacy was also observed on secondary efficacy measures, including the CGI-BP-S depression severity, and patient-rated measures of quality of life and functioning. In the second 6-week adjunctive trial, lurasidone was associated with significantly greater improvement in the MADRS starting at week 2 and continuing through week 5; significance was not maintained at week 6. In this study, significant improvement at endpoint was observed on the HAM-A, and on a patient-rated measure of quality of life. The most frequently reported adverse events in the three short-term studies were nausea, somnolence and akathisia. Low rates of weight gain and few effects on lipid and glucose parameters were observed. Treatment with lurasidone for 6 months was safe and well-tolerated with minimal effect on weight and metabolic parameters. Sustained improvement in depressive symptoms was observed during longer-term treatment.

Results

67 medication-free patients were enrolled, 49 patients were randomized (23 arm A, 26 arm B); 32 patients (16 A, 16 B) met evaluable criteria at 21 weeks. 41 of 67 enrolled patients met remission criteria at end of acute treatment (61.2%). At the 3-months, 10/16 patients (62.5%) (A) vs. 7/16 patients (43.8%) (B) did not experience symptomatic worsening. At the six-months, 15/16 patients (A) vs. 8/16 patients (B) remained in the study.

Results

A total of 256/1532 (16.7%) patients met criteria for prominent negative symptoms. Treatment of the prominent negative symptom group with lurasidone (vs. placebo) was associated with significantly greater week 6 improvement in the PANSS total score (−23.2 vs. −13.5; p<0.001), PANSS-negative subscale score (−6.3 vs. −4.5; p<0.01), and CGI-S (−1.3 vs. −0.8; p<0.001). Treatment of the prominent negative symptom group with lurasidone (vs. placebo) was associated with significantly greater endpoint response using the PANSS total 20% improvement criterion (69.2% vs. 51.5%; p<0.01; NNT=6), 30% criterion (54.1% vs. 34.0%; p<0.01; NNT=5), and 40% criterion (42.1% vs. 26.8%; p<0.05; NNT=7). In the group without prominent negative symptoms, treatment with lurasidone (vs. placebo) was associated with significantly greater endpoint responder rates using the PANSS 20% improvement criterion (62.3% vs. 43.4%; p<0.0001; NNT=6), 30% criterion (49.5% vs. 31.3%; p<0.0001; NNT=6), and 40% criterion (35.7% vs. 22.8%; p<0.0001; NNT=8). Discontinuation due to adverse events, for lurasidone vs. placebo, respectively, was low in both the prominent negative symptom group (6.3% vs. 2.1%) and the group without prominent negative symptoms (6.5% vs. 3.7%). In the prominent negative symptom group, the 3 most common adverse events reported for lurasidone (and greater than placebo) were headache (22.0% vs. 14.4%), somnolence (22.0% vs. 4.1%), and insomnia (18.2% vs. 16.5%).

Results

Mean (SD) 6 week QIDS-SR scores were 10.36 (6.18) and 12.97 (6.94) for the TMS and STAR*D populations, respectively (p<0.0001). Categorical outcomes at 6 weeks using the QIDS-SR definitions for none (0-5), mild (6-10), moderate (11-15) or moderate to severe (16-27) depression demonstrated that patients treated with TMS reported significantly greater clinical improvement compared to the STAR*D population (QIDS-SR total score <10: TMS, 53% vs STAR*D, 38%, P=0.0023, reverse matching method).

Results

TMS shows an incremental cost-effectiveness ratio (ICER) of $36,383/QALY. Mean annual costs were $11,886 and $10,888 for TMS and STAR*D patients, respectively. The estimated payment per member per month (PMPM) cost to provide TMS as a covered benefit for a moderate-sized payor comprised of 6,000,000 covered lives and assuming a 2% incidence of patients failing to benefit from initial medication, and a utilization of TMS of 15% among these patients was $0.25 over two years of treatment and follow up.

Results

A total of 1081 subjects entered the open-label aripiprazole once-monthly maintenance phase (464 from Study 246 [1], 474 from Study 247 [1] and 143 de novo subjects). Of these, 79.4% (858/1081) completed 52 weeks of treatment. The most frequent primary reasons for discontinuation were withdrawal of consent (8.2%), impending relapse (4%) [3.4% with adverse events plus 0.6% without adverse events], and adverse events (2.9%). Adverse events reported by? 5% of patients in the extension study were headache (7.6%), nasopharyngitis (7%), anxiety (6.8%), and insomnia (6.6%). The proportion of subjects in Phase 3 meeting impending relapse criteria (previously defined [1;2]) was 8.25% (89/1079).

Results

Of 433 patients in the efficacy analysis, 336 entered the 4th month of Phase B and were part of the primary efficacy outcome comparison. Hospitalization rates for patients receiving aripiprazole once-monthly 400 mg (2.7% [n=9/336]) were significantly lower than for the same patients previously treated with oral antipsychotics (27.1% [n=91/336]; P<0.0001). All-cause discontinuations during the entire prospective phase B were 32.3% (n=140/433). The most common reasons for discontinuation were patient withdrew consent (9.5% [n=41/433]), adverse events (8.5% [n=37/433]), and patient lost to follow-up (7.6% [n=33/433]). Adverse events with?5% incidence were insomnia (6.7% [n=29/431]) and akathisia (6.5% [n=28/431]).

Results

Preliminary outcomes are qualitative, finding more confidence in breadth of prescribing among novice PMHNPs, increased employer satisfaction with initial prescriptive skills, marketability of new PMHNP graduates, and plans for ongoing use of NEI membership as lifelong psychopharmacology learners. We anticipate enduring, improved learning outcomes and will evaluate trends in course grades, post-licensure board certification first-time pass rates, prescriber efficiency, as well as employer and patient satisfaction.

Results

At double-blind baseline, the prevalence of metabolic syndrome was similar in the lurasidone group (22.8%; 95/416) and risperidone group (23.4%; 47/201). After 12 months of treatment, metabolic syndrome prevalence (observed cases [OC]) was 20.8% (31/149) with lurasidone and 32.6% (30/92) with risperidone (p<0.05). In patients without metabolic syndrome at baseline, 14.0% (16/114) of lurasidone-treated patients and 21.4% (15/70) of risperidone-treated patients met criteria for metabolic syndrome after 12 months (OC); risk of developing metabolic syndrome was reduced by 40% with lurasidone relative to risperidone (odds ratio=0.60; 95% CI, 0.27-1.30). Among patients with metabolic syndrome at baseline, 55.9% (19/34) in the lurasidone group and 28.6% (6/21) in the risperidone group no longer met criteria for metabolic syndrome after 12 months (OC, p<0.05). The incidence of metabolic-related adverse events during the double-blind phase was 11.7% in the lurasidone group and 20.8% in the risperidone group. For patients who took lurasidone in both the double-blind and open-label phases (n=109, completers), metabolic syndrome prevalence was 20.2% at both open-label baseline and at open-label month 6. The prevalence of metabolic syndrome in patients switched to open-label lurasidone after 12 months of double-blind risperidone treatment (n=65, completers) was 33.8% at open-label baseline and decreased to 29.2% after 6 months of open-label lurasidone.

Results

The OLE study enrolled 136 patients continued on lurasidone (LUR-LUR) and 87 patients switched from risperidone (RIS-LUR). Mean lurasidone dose during the OLE was 81.1 mg/d. The OLE completion rate was 80.1% for LUR-LUR and 74.7% for RIS-LUR. During the double-blind study, mean weight increased (2.3 kg) in risperidone-treated patients who subsequently continued into the OLE but decreased in lurasidone-treated patients (−1.0 kg). During the OLE, mean (SD) change in weight was −0.6 kg (3.3 kg) for LUR-LUR and −2.9 kg (5.4 kg) for RIS-LUR patients (observed cases [OC]). For LUR-LUR patients, median changes in metabolic parameters from OLE baseline to endpoint (OC) were −4.0 mg/dL for total cholesterol, −4.5 mg/dL for triglycerides, and 0.0 mg/dL for glucose. For RIS-LUR patients, median changes in metabolic parameters from OLE baseline to endpoint (OC) were 4.5 mg/dL for total cholesterol, −5.5 mg/dL for triglycerides, and −3.0 mg/dL for glucose. During the double-blind study, median prolactin level increased in risperidone-treated patients who subsequently continued into the OLE (men, 12.8 ng/mL; women, 35.2 ng/mL), but levels decreased in lurasidone-treated patients (men, −0.6 ng/mL; women, −0.8 ng/mL). During the OLE, prolactin levels showed little change in LUR-LUR patients (median change from OLE baseline to endpoint [OC]: men, 0.2 ng/mL; women, 1.3 ng/mL) and decreased in RIS-LUR patients (men, −11.2 ng/mL; women, −30.8 ng/mL). During the OLE, 5.1% of LUR-LUR patients and 6.9% of RIS-LUR patients discontinued due to an adverse event (AE). Extrapyramidal symptom-related AEs were noted in 8.1% of LUR-LUR patients and 6.9% of RIS-LUR patients during the OLE. Akathisia and somnolence each occurred in 3.7% of LUR-LUR patients and 2.3% of RIS-LUR patients during the OLE. Mean (SD) Positive and Negative Syndrome Scale total score was 55.5 (12.7) at OLE baseline, and mean change at month 6 of the OLE was 0.6 in both the LUR-LUR and RIS-LUR groups (OC).

Results

Of the 676 patients enrolled in the open-label stabilization phase, 285 met stabilization criteria and were randomized to lurasidone (N=144) or placebo (N=141). Among randomized patients, mean PANSS total score decreased from 90.1 at open-label baseline to 54.4 at double-blind baseline, indicating substantial symptom improvement during the open-label phase. Time to relapse was significantly delayed (log-rank test, p=0.039), and the risk for relapse was reduced by 33.7% in lurasidone-treated patients versus patients in the placebo group (Cox model hazard ratio [95% CI], 0.663 [0.447–0.983]; p=0.041). Patients receiving placebo experienced significantly greater clinical worsening based on mean change in PANSS and CGI-S scores over the double-blind period compared with lurasidone-treated patients (PANSS, +12.4 vs +8.3 [p=0.029]; CGI-S, +0.7 vs +0.4 [p=0.015]; LOCF). The most common AEs reported in patients treated with lurasidone (open-label baseline through double-blind endpoint) were akathisia (16.7%), insomnia (12.5%), headache (11.8%), nausea (11.1%), and anxiety (11.1%). Discontinuation rates due to TEAEs in the double-blind phase were 13.9% for lurasidone and 15.6% for placebo. Lurasidone-treated patients experienced minimal changes in weight and prolactin, lipid, and glucose parameters throughout the study.

Results

Brex demonstrated subnanomolar binding affinities for 5-HT1A (Ki=0.12 nM), 5-HT2A (0.47), D2L (0.30), alpha1B (0.17), and alpha2C (0.59) receptors, with affinity of <5 nM at 5HT2B/7, D3 and alpha1A/1D receptors. In functional assays, brex acted as: a potent partial agonist at 5-HT1A and D2L/3; a moderate partial agonist at 5-HT2C; a potent antagonist at 5-HT2A/2B, alpha1A/1B/1D, and H1 and; a moderate antagonist at alpha2C. Consistent with in vitro binding affinities, receptor occupancy was in the following order of potency: D2>5-HT2A>5-HT1A>5-HT6>5-HT transporter>5-HT7. Oral brex (1-30 mg/kg) in rats increased brain levels of histamine in the medial prefrontal cortex and decreased dopamine levels in the nucleus accumbens but exerted no effect on the other neurotransmitters.

Results

Both service members underwent treatment. The first Marine was medically discharged and the second completed her enlistment and left active duty, but remains in the Reserves.

Results

Neither vortioxetine nor vortioxetine plus flesinoxan affected sexual behavior in male rats, whereas 2 weeks of paroxetine impaired sexual behavior significantly in several measures. Vortioxetine, 1 and 10 mg/kg, corresponded to 50 and 87% SERT occupancy, which matched occupancies seen at clinical doses (5-20 mg/day), as shown in human PET studies. Paroxetine produced approximately 90% SERT occupancy. Flesinoxan enhanced sexual function in male rats after acute and 1-week dosing, but not after 2 weeks’ treatment. Acute, 1-week and 2-week CP-94235 treatment significantly impaired sexual behavior. Ondansetron impaired ejaculation frequency only after 2 weeks of treatment.

Results

The risk of developing TESD for MDD or GAD patients without sexual dysfunction at baseline was not statistically significantly different between VOR (5-20mg/day) and PBO, with non-inferiority demonstrated for 5mg. The risk of developing TESD was higher with DUL compared to placebo or VOR 5 and 10mg. In the head-to-head comparison with ESC (NCT01364649), VOR 10-20mg was statistically significantly superior to ESC 10-20mg in improving TESD as measured by change from baseline in Changes in Sexual Functioning Questionnaire (CSFQ) total score. Of 447 patients enrolled, 348 completed the 8-week study (VOR, n=169/225 [75.1%]; ESC, n=179/222 [80.6%]). In the primary MMRM analysis, LS mean change from Baseline in CSFQ-14 total score was 6.6 in the ESC group and 8.8 in the VOR groups at Week 8. The LS mean difference of 2.2 (95% CI: 0.48-4.02) was statistically significant (p=0.013), demonstrating the improvement in sexual functioning for the VOR group was superior to the improvement in the ESC group. Numerically more VOR-treated patients demonstrated clinically meaningful improvements in sexual functioning (change from Baseline CSFQ-14 total score ≥3; OR=1.50; P=0.06) and shifted to normal sexual functioning during the study (OR=1.37; P=0.112), compared with ESC. MDD treatment response achieved with earlier antidepressants (citalopram, paroxetine and sertraline) was maintained in both groups. The AE profile for vortioxetine was similar to that seen in previous trials, with nausea, headache, and dizziness the most common AEs.

Results

In preclinical studies vortioxetine led to changes in the function of several neurotransmitter systems including 5-HT, norepinephrine, dopamine, acetylcholine, histamine, gamma butyric acid (GABA) and glutamate in the rat brain. These effects likely derive from its interaction with serotonin receptor-mediated negative feedback mechanisms controlling neuronal activity of these brain areas, which is differentfrom the mechanism of action of current antidepressants, such as SSRIs. Studies in rodents revealed a differentiated profile in models predictive of antidepressant activity, increased synaptic plasticity and improved cognitive function compared to SSRIs and SNRIs. Furthermore, vortioxetine showed reduced interference with sexual function and sleep architecture compared to SSRIs in rats.

In placebo-controlled clinical trials of adults with MDD, vortioxetine (VOR) was efficacious in reducing depressive symptoms vs placebo (and vs agomelatine in a trial of patients with an inadequate response to SSRI/SNRI treatment) and was significantly superior to placebo in pre-defined cognitive outcomes. In a pooled analysis of patients treated with placebo (n=1621) or VOR (5-20mg/day) (n=2616), the incidence of insomnia-related AEs was 2.0–5.1% for VOR vs placebo (4.4%) and sexual dysfunction-related AEs was 1.6-2.6% for VOR vs placebo (1.1%). In a sleep EEG study with healthy subjects, VOR at a given SERT occupancy seemed to affect REM sleep less than paroxetine. In a pooled analysis of 7 clinical trials, the risk of developing treatment-emergent sexual dysfunction was not significantly different between VOR (5-20 mg/day) and placebo using the Arizona Sexual Experience Scale (ASEX). MDD patients treated with VOR experienced a significantly greater improvement in the Changes in Sexual Functioning Questionnaire (CSFQ-14) total score compared to escitalopram in a head-to-head study.

Results

We present here the first year findings. Most patients were men, single with secondary school grades. Regarding schizophrenia symptoms, 80% of patients experienced prodromal symptoms with a median duration of 426 days (IR 90-914), before the schizophrenia diagnosis were made the patients experimented a median of 423 days of psychotic symptoms (IR 77-823).

Before entering to the cohort the patients were experienced a median of 2 psychotic episodes (IR 2-4), and 2 psychiatric hospitalizations (IR 2-4). The rate of substance use observed in patients was 36%, and the main substance of abuse was cannabis.

The treatment in the patients were as follow: most patients were with atypical antipsychotic (96%), 16% were in treatment with depot medication. 64% of patients were receiving concomitant medications. And just 8% of patients were receiving any kind of non pharmacological treatment.

Satisfaction with medication was negative in 14%, neutral in 20% and positive in most patients (66%). Adherence to treatment was described by patient and relatives as high (average 88%).

Most patients were described as mild to without clinical compromise according to CGI-S, patients exhibit mild to moderate compromise in functioning as median values of PSP were 55 (IR 45-60) and GAF 55 (IR 50-65). During the first year of follow up one third of patients experienced at least one relapse of psychotic symptoms and they expended an average of 24 days with psychotic symptoms. 3 patients attempted against their lives and 2 committed suicide.

Results

At baseline, BPD participants exhibited significantly higher levels of myo-inositol (Ins) than HCS when co-varying for gray and white matter (p=0.042). Eight BPD participants received placebo treatment for eight weeks and seven received quetiapine. No significant differences were found between the baseline and exit metabolite levels in the placebo group. Following treatment with Quetiapine, creatine (Cr; t(6)=2.560; p=0.043) and glutamate/glutamine (Glx; t(6)=2.721, p=0.035) levels decreased.

Results

In oocytes from Xenopus laevis, encenicline significantly increased ion currents through α7 receptors. Further, encenicline promoted the release of ACh and glutamate (Glu) in the medial prefrontal cortex (mPFC), whereas dopamine (DA) release was enhanced in both the mPFC and the nucleus accumbens. An α7 receptor antagonist blocked encenicline-induced release of DA and Glu, and partially blocked the release of ACh. Cognitive testing in the rat demonstrated that encenicline improved memory performance in an object recognition task. Encenicline elicited the effects on cognition and neurotransmitter efflux in vivo at sub-nanomolar doses. Interestingly, administration of encenicline followed an inverted U-shaped dose-response curve for both measures of cognition and neurotransmitter efflux, such that higher doses resulted in diminished cognitive improvements and neurotransmitter release.

Results

The OCI plus Trails 2 and 4 suggested that versus placebo, 0.3 mg encenicline was associated with significant improvement in general cognitive function (P=0.009) due mainly to the improvements in visual learning, visual attention, and social cognition. The positive effect on the OCI was supported by a trend for improved cognition on the MCCB (P=0.069) in the 1 mg dose group. For the 1 mg group, the mean change from baseline at day 84 in the overall Composite T-score and the associated percentile change were higher than for the 0.3 mg and placebo groups. There were no clinically significant safety findings. A total of 192 treatment-emergent adverse events were reported in 101 (31.9%) subjects. The incidence of serious adverse events was similar among all treatment groups; none was judged related to drug. Significant improvements in clinical function were observed with encenicline as measured by the SCoRS at all visits for the 1 mg group versus placebo (P=0.011), and a significant effect on Negative Symptoms in the 1 mg group (P=0.028) was observed versus placebo on Day 77.

Results

In the individual studies, all cariprazine dose groups showed superiority to placebo (P<.05) on mean change from baseline to Week 6 in CGI-S scores. Least square mean differences (LSMD) ranged from −0.3 to −0.6. The pooled population comprised 161 patients (placebo, n=50; cariprazine, n=111) that were classified as severely or extremely ill and 1033 patients (placebo, n=311; cariprazine, n=722) that were at least markedly ill. A significantly greater proportion of severely ill patients at baseline improved to mildly ill or better in the cariprazine group compared with placebo (42% vs 18%; OR=3.43 [95% CI: 1.5, 7.9]; P=.004). In patients who were markedly ill or worse at baseline, 7% of cariprazine vs 3% of placebo patients improved to borderline ill/normal at Week 6 (OR=2.33 [95% CI: 1.1, 4.8]; P=.022).

Results

At baseline, 97 patients (placebo, n=42; cariprazine, n=55) were severely or extremely ill, 637 patients (placebo, n=254; cariprazine, n=383) were at least markedly ill, and 1033 (placebo, n=428; cariprazine, n=605) were at least moderately ill. A significantly greater percentage of cariprazine vs placebo patients improved from moderately ill or worse at baseline to borderline ill/normal at Week 3 (32% vs 22%; OR=1.71; P<.001). Similarly, a greater percentage of cariprazine vs placebo patients shifted from markedly ill or worse to borderline ill/normal (markedly ill: 32% vs 18%; OR=2.10; P<.001). A greater proportion of cariprazine vs placebo patients shifted from severely or extremely ill to mildly ill or better (55% vs 36%; odds ratio [OR]=2.12; P=.09) but differences did not reach statistical significance, probably due to small sample size.

Results

DM, the non-opioid d-isomer of levorphanol, is a low affinity, uncompetitive N-methyl-D-aspartate (NMDA) receptor antagonist with IC50 and Kd values ranging from 0.6 μM to 11 μM for blocking sustained NMDA-induced calcium or barium currents. DM has relatively rapid NMDA receptor dissociation kinetics which may be significant for tolerability. DM also inhibited ligand binding to SERT with a Ki=40 nM, has been shown to be relatively potent inhibitor of serotonin reuptake into rat brain synaptosomes in vitro (Ki=0.023 μM), and appears to inhibit serotonin reuptake in other animal models. It is a potent sigma-1 receptor agonist (Ki=200 nM), which has been indicated to be at least partly responsible for antidepressant-like activity of DM in the mouse forced swim test. DM weakly inhibits binding at the norepinephrine transporter (Ki=6-13 μM), but effectively inhibits the reuptake of norepinephrine (Ki=240 nM). Potential actions at other receptors, such as presynaptic antagonism of nicotinic acetylcholine receptors, are considered. Clinical efficacy appears driven by DM despite higher total DX exposure even in presence of Q. This may be due to the rapid conjugation and renal elimination of DX (lower CNS bioavailability) and differential activity at some key receptors. DM administration without Q metabolic inhibition is largely ineffective.

Results

In >40 patients thus treated over 3 years, all experienced an increased duration of sleep, less awakenings, and less fatigue. Subsequently tpp was reduced, as was fatigue, headache and stiffness. The FIQR significantly improved. Also both concentration/memory are improved and gradually so is the y to focus on a goal and accomplish it. Their response to various concomitant psychiatric therapies was improved - as demonstrated by a lessening of their anxiety/depression.