Your search keyword '"Giordano, Annalisa"' showing total 4 results

1. Cognitive function in early-phase schizophrenia-spectrum disorder: IQ subtypes, brain volume and immune markers.

Author

Watson, Andrew J., Giordano, Annalisa, Suckling, John, Barnes, Thomas R. E., Husain, Nusrat, Jones, Peter B., Krynicki, Carl R., Lawrie, Stephen M., Lewis, Shôn, Nikkheslat, Naghmeh, Pariante, Carmine M., Upthegrove, Rachel, Deakin, Bill, Dazzan, Paola, and Joyce, Eileen M.

Subjects

*BRAIN anatomy, *BIOMARKERS, *C-reactive protein, *INTERLEUKINS, *SCHIZOPHRENIA, *PSYCHOSES, *COGNITIVE processing speed, *COGNITION, *IMMUNE system, *MAGNETIC resonance imaging, *NEUROINFLAMMATION, *INTELLECT, *TUMOR necrosis factors, *VERBAL behavior, *RESEARCH funding

Abstract

Background: Evidence suggests that cognitive subtypes exist in schizophrenia that may reflect different neurobiological trajectories. We aimed to identify whether IQ-derived cognitive subtypes are present in early-phase schizophrenia-spectrum disorder and examine their relationship with brain structure and markers of neuroinflammation. Method: 161 patients with recent-onset schizophrenia spectrum disorder (<5 years) were recruited. Estimated premorbid and current IQ were calculated using the Wechsler Test of Adult Reading and a 4-subtest WAIS-III. Cognitive subtypes were identified with k-means clustering. Freesurfer was used to analyse 3.0 T MRI. Blood samples were analysed for hs-CRP, IL-1RA, IL-6 and TNF- α. Results: Three subtypes were identified indicating preserved (PIQ), deteriorated (DIQ) and compromised (CIQ) IQ. Absolute total brain volume was significantly smaller in CIQ compared to PIQ and DIQ, and intracranial volume was smaller in CIQ than PIQ (F (2, 124) = 6.407, p = 0.002) indicative of premorbid smaller brain size in the CIQ group. CIQ had higher levels of hs-CRP than PIQ (F (2, 131) = 5.01, p = 0.008). PIQ showed differentially impaired processing speed and verbal learning compared to IQ-matched healthy controls. Conclusions: The findings add validity of a neurodevelopmental subtype of schizophrenia identified by comparing estimated premorbid and current IQ and characterised by smaller premorbid brain volume and higher measures of low-grade inflammation (CRP). [ABSTRACT FROM AUTHOR]

Published

2023

2. Neurological Signs at the First Psychotic Episode as Correlates of Long-Term Outcome: Results From the AESOP-10 Study.

Author

Ferruccio, Naika P, Tosato, Sarah, Lappin, Julia M, Heslin, Margaret, Donoghue, Kim, Giordano, Annalisa, Lomas, Ben, Reininghaus, Ulrich, Onyejiaka, Adanna, Chan, Raymond C K, Croudace, Tim, Jones, Peter B, Murray, Robin M, Fearon, Paul, Doody, Gillian A, Morgan, Craig, and Dazzan, Paola

Subjects

LONGITUDINAL method, MOTOR ability, PSYCHOLOGY of movement, NEUROLOGICAL disorders, PSYCHOSES, DESCRIPTIVE statistics

Abstract

Minor neurological signs are subtle deficits in sensory integration, motor coordination, and sequencing of complex motor acts present in excess in the early stages of psychosis. Still, it remains unclear whether at least some of these signs represent trait or state markers for psychosis and whether they are markers of long-term disease outcome of clinical utility. We examined the relationship between neurological function at illness onset assessed with the Neurological Evaluation Scale and subsequent illness course in 233 patients from AESOP-10 (Aetiology and Ethnicity in Schizophrenia and Other Psychoses), a 10-year follow-up study of a population-based cohort of individuals recruited at the time of their first episode of psychosis in the United Kingdom. In 56 of these patients, we also explored changes in neurological function over time. We included a group of 172 individuals without psychosis as controls. After 10 years, 147 (63%) patients had developed a non-remitting course of illness, and 86 (37%) a remitting course. Already at first presentation, patients who developed a non-remitting course had significantly more primary, motor coordination, and total signs than both remitting patients and healthy controls. While Motor Coordination signs did not change over time, rates of Primary, Sensory Integration, and Total signs increased, independently of illness course type. These findings suggest that motor coordination problems could be a useful early, quick, and easily detectable marker of subsequent clinical outcome. With other motor abnormalities, a measure of motor incoordination could contribute to the identification of the most vulnerable individuals, who could benefit from targeted and more assertive treatment approaches. [ABSTRACT FROM AUTHOR]

Published

2021

3. Cortisol and Inflammatory Biomarkers Predict Poor Treatment Response in First Episode Psychosis.

Author

Mondelli, Valeria, Ciufolini, Simone, Murri, Martino Belvederi, Bonaccorso, Stefania, Di Forti, Marta, Giordano, Annalisa, Marques, Tiago R., Zunszain, Patricia A., Morgan, Craig, Murray, Robin M., Pariante, Carmine M., and Dazzan, Paola

Subjects

DRUG therapy for psychoses, BIOMARKERS, CORTISONE, CYTOKINES, ENZYME-linked immunosorbent assay, INFLAMMATION, INTERLEUKINS, PROBABILITY theory, PSYCHOLOGICAL tests, PSYCHOSES, RESEARCH funding, SALIVA, STATISTICS, DATA analysis, REPEATED measures design, DATA analysis software, ONE-way analysis of variance

Abstract

Background: Cortisol and inflammatory markers have been increasingly reported as abnormal at psychosis onset. The main aim of our study was to investigate the ability of these biomarkers to predict treatment response at 12 weeks follow-up in first episode psychosis. Methods: In a longitudinal study, we collected saliva and blood samples in 68 first episode psychosis patients (and 57 controls) at baseline and assessed response to clinician-led antipsychotic treatment after 12 weeks. Moreover, we repeated biological measurements in 39 patients at the same time we assessed the response. Saliva samples were collected at multiple time points during the day to measure diurnal cortisol levels and cortisol awakening response (CAR); interleukin (IL)-1β, IL-2, IL-4, IL-6, IL-8, IL-10, tumor necrosis factor-α, and interferon-γ (IFN-γ) levels were analyzed from serum samples. Patients were divided into Non-Responders (n = 38) and Responders (n = 30) according to the Remission symptom criteria of the Schizophrenia Working Group Consensus. Results: At first onset, Non- Responders had markedly lower CAR (d = 0.6, P = .03) and higher IL-6 and IFN-γ levels (respectively, d = 1.0, P = .003 and d = 0.9, P = .02) when compared with Responders. After 12 weeks, Non-Responders show persistent lower CAR (P = .01), and higher IL-6 (P = .04) and IFN-γ (P = .05) when compared with Responders. Comparison with controls show that these abnormalities are present in both patients groups, but are more evident in Non-Responders. Conclusions: Cortisol and inflammatory biomarkers at the onset of psychosis should be considered as possible predictors of treatment response, as well as potential targets for the development of novel therapeutic agents. [ABSTRACT FROM AUTHOR]

Published

2015

4. Cortical Folding Defects as Markers of Poor Treatment Response in First-Episode Psychosis.

Author

Palaniyappan, Lena, Marques, Tiago Reis, Taylor, Heather, Handley, Rowena, Mondelli, Valeria, Bonaccorso, Stefania, Giordano, Annalisa, McQueen, Grant, DiForti, Marta, Simmons, Andrew, David, Anthony S., Pariante, Carmine M., Murray, Robin M., and Dazzan, Paola

Subjects

PSYCHOSES, BRAIN imaging, ANTIPSYCHOTIC agents, NEURODEVELOPMENTAL treatment, DIAGNOSIS, MEDICAL history taking

Abstract

IMPORTANCE: At present, no reliable predictors exist to distinguish future responders from nonresponders to treatment during the first episode of psychosis. Among potential neuroimaging predictors of treatment response, gyrification represents an important marker of the integrity of normal cortical development that may characterize, already at illness onset, a subgroup of patients with particularly poor outcome. OBJECTIVE: To determine whether patients with first-episode psychosis who do not respond to 12 weeks of antipsychotic treatment already have significant gyrification defects at illness onset. DESIGN: Case-control study with 12 weeks' longitudinal follow-up to determine treatment response. SETTING: Secondary psychiatric services in an inner-city area (South London, England). PARTICIPANTS: A total of 126 subjects, including 80 patients presenting with first-episode psychosis and 46 healthy controls. Patients were scanned at the outset and received various antipsychotic medications in a naturalistic clinical setting. They were followed up for 12 weeks and classified as responders or nonresponders if they reached criteria for symptom remission, evaluated with the Psychiatric and Personal History Schedule. OBSERVATION: Patients were exposed to naturalistic antipsychotic treatment for 12 weeks following amagnetic resonance imaging scan. MAIN OUTCOMES AND MEASURES: Cortical gyrificationwas assessed using local gyrification index in a vertexwise fashion across the entire cortical surface with correction for multiple testing using permutation analysis. Differences in local gyrification index were assessed between responders, nonresponders, and healthy controls. The effect of diagnosis (affective vs nonaffective psychosis) on the local gyrification index was also investigated in responders and nonresponders. RESULTS: Patients with first-episode psychosis showed a significant reduction in gyrification (hypogyria) across multiple brain regions compared with healthy controls. Interestingly, nonresponders showed prominent hypogyria at bilateral insular, left frontal, and right temporal regions when compared with responders (all clusters significant at P < .05). These effects were present for both affective and nonaffective psychoses. CONCLUSIONS AND RELEVANCE: Gyrification appears to be a useful predictor of antipsychotic treatment response. Early neurodevelopmental aberrations may predict unfavorable prognosis in psychosis, irrespective of the existing diagnostic boundaries. [ABSTRACT FROM AUTHOR]

Published

2013