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2. Association of hospitalization with structural brain alterations in patients with affective disorders over nine years

Author

Förster, Katharina, Grotegerd, Dominik, Dohm, Katharina, Lemke, Hannah, Enneking, Verena, Meinert, Susanne, Redlich, Ronny, Heindel, Walter, Bauer, Jochen, Kugel, Harald, Suslow, Thomas, Ohrmann, Patricia, Carballedo, Angela, O’Keane, Veronica, Fagan, Andrew, Doolin, Kelly, McCarthy, Hazel, Kanske, Philipp, Frodl, Thomas, and Dannlowski, Udo

Published
2023
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4. Association of hospitalization with structural brain alterations in patients with affective disorders over nine years

Author

Katharina Förster, Dominik Grotegerd, Katharina Dohm, Hannah Lemke, Verena Enneking, Susanne Meinert, Ronny Redlich, Walter Heindel, Jochen Bauer, Harald Kugel, Thomas Suslow, Patricia Ohrmann, Angela Carballedo, Veronica O’Keane, Andrew Fagan, Kelly Doolin, Hazel McCarthy, Philipp Kanske, Thomas Frodl, and Udo Dannlowski

Subjects
Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571
Abstract

Abstract Repeated hospitalizations are a characteristic of severe disease courses in patients with affective disorders (PAD). To elucidate how a hospitalization during a nine-year follow-up in PAD affects brain structure, a longitudinal case-control study (mean [SD] follow-up period 8.98 [2.20] years) was conducted using structural neuroimaging. We investigated PAD (N = 38) and healthy controls (N = 37) at two sites (University of Münster, Germany, Trinity College Dublin, Ireland). PAD were divided into two groups based on the experience of in-patient psychiatric treatment during follow-up. Since the Dublin-patients were outpatients at baseline, the re-hospitalization analysis was limited to the Münster site (N = 52). Voxel-based morphometry was employed to examine hippocampus, insula, dorsolateral prefrontal cortex and whole-brain gray matter in two models: (1) group (patients/controls)×time (baseline/follow-up) interaction; (2) group (hospitalized patients/not-hospitalized patients/controls)×time interaction. Patients lost significantly more whole-brain gray matter volume of superior temporal gyrus and temporal pole compared to HC (p FWE = 0.008). Patients hospitalized during follow-up lost significantly more insular volume than healthy controls (p FWE = 0.025) and more volume in their hippocampus compared to not-hospitalized patients (p FWE = 0.023), while patients without re-hospitalization did not differ from controls. These effects of hospitalization remained stable in a smaller sample excluding patients with bipolar disorder. PAD show gray matter volume decline in temporo-limbic regions over nine years. A hospitalization during follow-up comes with intensified gray matter volume decline in the insula and hippocampus. Since hospitalizations are a correlate of severity, this finding corroborates and extends the hypothesis that a severe course of disease has detrimental long-term effects on temporo-limbic brain structure in PAD.

Published
2023
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5. An observational treatment study of metacognition in anxious-depression

Author

Celine Ann Fox, Chi Tak Lee, Anna Kathleen Hanlon, Tricia XF Seow, Kevin Lynch, Siobhán Harty, Derek Richards, Jorge Palacios, Veronica O'Keane, Klaas Enno Stephan, and Claire M Gillan

Subjects
metacognition, confidence, anxious-depression, transdiagnostic, iCBT, antidepressant, Medicine, Science, Biology (General), QH301-705.5
Abstract

Prior studies have found metacognitive biases are linked to a transdiagnostic dimension of anxious-depression, manifesting as reduced confidence in performance. However, previous work has been cross-sectional and so it is unclear if under-confidence is a trait-like marker of anxious-depression vulnerability, or if it resolves when anxious-depression improves. Data were collected as part of a large-scale transdiagnostic, four-week observational study of individuals initiating internet-based cognitive behavioural therapy (iCBT) or antidepressant medication. Self-reported clinical questionnaires and perceptual task performance were gathered to assess anxious-depression and metacognitive bias at baseline and 4-week follow-up. Primary analyses were conducted for individuals who received iCBT (n=649), with comparisons between smaller samples that received antidepressant medication (n=82) and a control group receiving no intervention (n=88). Prior to receiving treatment, anxious-depression severity was associated with under-confidence in performance in the iCBT arm, replicating previous work. From baseline to follow-up, levels of anxious-depression were significantly reduced, and this was accompanied by a significant increase in metacognitive confidence in the iCBT arm (β=0.17, SE=0.02, p

Published
2023
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6. The Precision in Psychiatry (PIP) study: Testing an internet-based methodology for accelerating research in treatment prediction and personalisation

Author

Chi Tak Lee, Jorge Palacios, Derek Richards, Anna K. Hanlon, Kevin Lynch, Siobhan Harty, Nathalie Claus, Lorraine Swords, Veronica O’Keane, Klaas E Stephan, and Claire M Gillan

Subjects
Treatment response, Treatment outcomes, Treatment prediction, Mental health treatments, Internet-based methodology, Big data, Psychiatry, RC435-571
Abstract

Abstract Background Evidence-based treatments for depression exist but not all patients benefit from them. Efforts to develop predictive models that can assist clinicians in allocating treatments are ongoing, but there are major issues with acquiring the volume and breadth of data needed to train these models. We examined the feasibility, tolerability, patient characteristics, and data quality of a novel protocol for internet-based treatment research in psychiatry that may help advance this field. Methods A fully internet-based protocol was used to gather repeated observational data from patient cohorts receiving internet-based cognitive behavioural therapy (iCBT) (N = 600) or antidepressant medication treatment (N = 110). At baseline, participants provided > 600 data points of self-report data, spanning socio-demographics, lifestyle, physical health, clinical and other psychological variables and completed 4 cognitive tests. They were followed weekly and completed another detailed clinical and cognitive assessment at week 4. In this paper, we describe our study design, the demographic and clinical characteristics of participants, their treatment adherence, study retention and compliance, the quality of the data gathered, and qualitative feedback from patients on study design and implementation. Results Participant retention was 92% at week 3 and 84% for the final assessment. The relatively short study duration of 4 weeks was sufficient to reveal early treatment effects; there were significant reductions in 11 transdiagnostic psychiatric symptoms assessed, with the largest improvement seen for depression. Most participants (66%) reported being distracted at some point during the study, 11% failed 1 or more attention checks and 3% consumed an intoxicating substance. Data quality was nonetheless high, with near perfect 4-week test retest reliability for self-reported height (ICC = 0.97). Conclusions An internet-based methodology can be used efficiently to gather large amounts of detailed patient data during iCBT and antidepressant treatment. Recruitment was rapid, retention was relatively high and data quality was good. This paper provides a template methodology for future internet-based treatment studies, showing that such an approach facilitates data collection at a scale required for machine learning and other data-intensive methods that hope to deliver algorithmic tools that can aid clinical decision-making in psychiatry.

Published
2023
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7. Core‐shell encapsulation formulations to stabilize desiccated Bradyrhizobium against high environmental temperature and humidity

Author

Kelly G. Aukema, Mian Wang, Beatriz deSouza, Sophie O'Keane, Maia Clipsham, Lawrence P. Wackett, and Alptekin Aksan

Subjects
Biotechnology, TP248.13-248.65
Abstract

Summary Engineered materials to improve the shelf‐life of desiccated microbial strains are needed for cost‐effective bioaugmentation strategies. High temperatures and humidity of legume‐growing regions challenge long‐term cell stabilization at the desiccated state. A thermostable xeroprotectant core and hydrophobic water vapour barrier shell encapsulation technique was developed to protect desiccated cells from the environment. A trehalose core matrix increased the stability of desiccated Bradyrhizobium by three orders of magnitude over 20 days at 32°C and 50% relative humidity (RH) compared to buffer alone; however, the improvement was not deemed sufficient for a shelf‐stable bioproduct. We tested common additives (skim milk, albumin, gelatin and dextran) to increase the glass transition temperature of the desiccated product to provide further stabilization. Albumin increased the glass transition temperature of the trehalose‐based core by 40°C and stabilized desiccated Bradyrhizobium for 4 months during storage at high temperature (32°C) and moderate humidity (50% RH) with only 1 log loss of viability. Although the albumin‐trehalose core provided exceptional protection against high temperature, it was ineffective at higher humidity conditions (75%). We therefore incorporated a paraffin shell, which protected desiccated cells against 75% RH providing proof of concept that core and shell encapsulation is an effective strategy to stabilize desiccated cells.

Published
2022
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10. Glomangiomatosis of the lower leg

Author

David Glynn, DG FFRRCSI, John Hynes, JH FFRRCSI, Kate Richards, KR MB BCh, Gary O'Toole, GOT FRCS(Tr&Orth), Conor O'Keane, COK MRCPI, and Eoin Kavanagh, EK FFRRCSI

Subjects
Glomangioma, Glomangiomatosis, Atypical glomus tumor, Soft tissue masses, Medical physics. Medical radiology. Nuclear medicine, R895-920
Abstract

This paper demonstrates a case of multiple glomangiomas, or glomangiomatosis, including clinical presentation, imaging appearances, and subsequent management. Differentiating features from typical glomus tumors are described. To the best of our knowledge, this is the first reported case of a glomangioma involving the distal tibiofibular syndesmosis.

Published
2022
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11. A case of multiple metastases from a primary renal solitary fibrous tumour; The uncertain long road.

Author

C Ward, Z Tsvetanova, C O'Keane, and D O'Mahony

Subjects
Solitary Fibrous Tumour, Kidney, Pulmonary, Metastatic, Resection, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Solitary fibrous tumours (SFT) comprise a rare subset of soft tissue tumours of mesenchymal origin accounting for fewer than 2% of all soft tissue tumours, most commonly arising in the pleura (Davanzo et al., 2018). The kidney as a primary site is extremely uncommon (Znati et al., 2007). The majority of SFT's exhibit indolent behaviour although local or distant recurrence may occur in 10-30% of cases (Fletcher, 2013). Those with malignant features such as mitotic rate more than 4 mitoses per 10 high power fields (>4/10 HPF) represent a much greater risk of recurrence (England, Hochholzer and McCarthy, 1989). Here we present an unusual case of a patient who presented with multiple metastatic recurrences of a SFT of primary renal origin spanning over 2 decades. The original tumour was small with benign features and clear margins of resection. 15 years later she presented with a pulmonary recurrence which was again resected with clear margins. A further pulmonary metastasis with bland features was resected 5 years later. Given such prognostic indicators our patient not surprisingly enjoyed a long disease-free interval of 15 years. Sequential resection of localized metastases provided further survival benefit of 5 years until the development of disseminated metastatic disease. Our case highlights the unpredictable nature of SFT's even in the setting of such favourable prognostic features. We discuss recent advances in the management of metastatic SFTs. Although the data regarding the use of systemic therapy in this setting is ill-defined, there remains sufficient evidence to suggest potential benefit in this case.

Published
2022
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12. Tenosynovial chondromatosis of the flexor pollicis longus tendon: A subtype of primary synovial chondromatosis

Author

Alexandra Murphy, Mb BCH BAO MRCPI FFR RCSI, Bryan Yelverton, Bsc MB BCh BAO, Danilo Vukanic, MB BCh BAO MCh MRCSI, Zornitsa Tsvetanova, MD, MD, MSc, Sarah-Kate Eustace, Medical Student, Alan Molloy, Mb BCh, Conor J O'Keane, FFPath FRCPI, and Eoin Kavanagh, FFR RCSI

Subjects
Tenosynovial chondromatosis, Thumb, Tendon sheath synovial chondromatosis, Flexor pollicis longus tendon, Synovectomy, Medical physics. Medical radiology. Nuclear medicine, R895-920
Abstract

Primary synovial chondromatosis is a rare benign neoplastic process, in which cartilaginous nodules are produced in the subsynovial tissue. It has 3 main subtypes (intra-articular, tenosynovial and bursal). We present the case of a 61-year-old female, with a mass involving her right thumb for at least 5 years, which had recently increased in size. X-ray showed a soft tissue mass, without calcification or any underlying bony abnormality. Ultrasound and MRI showed a 6-cm mass surrounding the right flexor pollicis longus tendon of the right thumb. The patient went on to have surgical resection and was given a diagnosis of tenosynovial chondromatosis.

Published
2021
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14. Multimodal imaging of Spina Ventosa (TB Dactylitis) of the foot

Author

Mark C. Murphy, MB, Bch, Bao, Alexandra N. Murphy, MB, Bch, Bao, Hannah Hughes, MB, Bch, Bao, Owen J. McEneaney, MB, Bch, BAO, Conor O'Keane, MB, Bch, BAO, and Eoin Kavanagh, MB, Bch, BAO

Subjects
TB dactylitis, Spina Ventosa, Osteomyelitis, Medical physics. Medical radiology. Nuclear medicine, R895-920
Abstract

We present the case of a 29-year-old male healthcare worker with a 6 month history of progressive left foot pain resulting in presentation to the emergency department on 3 occasions. He denied systemic symptoms. Multimodal imaging demonstrated an expansile erosive inflammatory lesion centered on the neck of the second metatarsal with aggressive features. CT of the thorax, abdomen, and pelvis demonstrated calcified mediastinal lymph nodes and left inguinal adenopathy. The lesion was biopsied under ultrasound guidance demonstrating a necrotizing granulomatous osteomyelitis with acid fact bacilli. This is consistent with TB dactylitis (spina ventosa). Treatment with antimycobacterial drugs was commenced.

Published
2020
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15. The human dorsal hippocampal commissure: Delineating connections across the midline using multi-modal neuroimaging in major depressive disorder

Author

Anurag Nasa, Caoimhe Gaughan, Muhammad Mahmoud, John R. Kelly, Elena Roman, Kirk J. Levins, Denis Barry, Thomas Frodl, Erik O'Hanlon, Veronica O'Keane, and Darren William Roddy

Subjects
Dorsal hippocampal commissure, Major depressive disorder, Diffusion weighted imaging, Parahippocampal gyrus, Hippocampus, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571
Abstract

Reclining on the lyra of the fornix, the dorsal hippocampal commissure (DHC) facilitates communication between the left and right hippocampi. Despite being a key commissural fiber bundle of the hippocampus, the DHC remains relatively underexplored in humans. Using high-resolution T1 and T2 magnetic resonance imaging in conjunction with High Angular Resolution Diffusion Imaging and Constrained Spherical Deconvolution tractography, we investigated if there are differences between the DHC of a sample of 54 healthy controls and 38 patients diagnosed with Major Depressive Disorder (MDD). After isolating the DHC using an anatomically derived protocol, segmented volumes of the left and right temporal pole, amygdala, hippocampus and parahippocampal gyrus extracted. In both controls and MDD patients, DHC fibers were spread across each of these four regions, with the parahippocampal gyri contributing the most to the volume of this white matter tract. Furthermore, diffusion metrics showed no effect of aging or sex on the integrity of the DHC in either group. This study is the first to investigate the DHC in MDD and the first to demonstrate that the DHC connects with the amygdala and temporal pole on both sides of the brain. Our data shows that the human DHC, rather than simply connecting the left and right hippocampi, allows connections between each hippocampus and the contralateral temporal pole, amygdala and parahippocampal gyrus. This suggests that the human temporal lobe, and the parahippocampal gyrus, may exert more influence on the contralateral limbic system via the DHC than previously thought.

Published
2021
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16. Psychedelic Therapy's Transdiagnostic Effects: A Research Domain Criteria (RDoC) Perspective

Author

John R. Kelly, Claire M. Gillan, Jack Prenderville, Clare Kelly, Andrew Harkin, Gerard Clarke, and Veronica O'Keane

Subjects
psychedelics, hallucinogens, psilocybin, research domain criteria (RDoC), lysergic acid diethylamide (LSD), dimethyltryptamine (DMT), Psychiatry, RC435-571
Abstract

Accumulating clinical evidence shows that psychedelic therapy, by synergistically combining psychopharmacology and psychological support, offers a promising transdiagnostic treatment strategy for a range of disorders with restricted and/or maladaptive habitual patterns of emotion, cognition and behavior, notably, depression (MDD), treatment resistant depression (TRD) and addiction disorders, but perhaps also anxiety disorders, obsessive-compulsive disorder (OCD), Post-Traumatic Stress Disorder (PTSD) and eating disorders. Despite the emergent transdiagnostic evidence, the specific clinical dimensions that psychedelics are efficacious for, and associated underlying neurobiological pathways, remain to be well-characterized. To this end, this review focuses on pre-clinical and clinical evidence of the acute and sustained therapeutic potential of psychedelic therapy in the context of a transdiagnostic dimensional systems framework. Focusing on the Research Domain Criteria (RDoC) as a template, we will describe the multimodal mechanisms underlying the transdiagnostic therapeutic effects of psychedelic therapy, traversing molecular, cellular and network levels. These levels will be mapped to the RDoC constructs of negative and positive valence systems, arousal regulation, social processing, cognitive and sensorimotor systems. In summarizing this literature and framing it transdiagnostically, we hope we can assist the field in moving toward a mechanistic understanding of how psychedelics work for patients and eventually toward a precise-personalized psychedelic therapy paradigm.

Published
2021
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19. Subperiosteal hematoma of the iliac wing presenting with leg weakness in a young adult footballer

Author

John P. Hynes, MB, BCH, BAO, Richard E. Downey, MB, BCH, BAO, MScSEM, Nicola Hughes, FRCR, Conor J. O'Keane, FRCPath, and Eoin Kavanagh, FRCR

Subjects
Medical physics. Medical radiology. Nuclear medicine, R895-920
Abstract

We present the case of a 17 year old football player with a 2 week history of left leg weakness and difficulty weight-bearing. Magnetic resonance imaging revealed a well-circumscribed lesion deep to the left iliacus muscle. The patient proceeded to computed tomography-guided biopsy. The likely diagnosis was that of a subperiosteal haematoma of the iliac wing, which was exerting mass effect upon the left femoral nerve resulting in leg pain and weakness. Imaging was repeated at an interval of 1 month, at which time the lesion had almost entirely resolved. Subperiosteal haematoma of the iliac bone is a rare entity but should be considered as a potential diagnosis in young adults, particularly where there is a history of trauma or recent sports injury. Keywords: Subperiosteal haematoma, Iliac bone, Femoral neuropathy, Magnetic resonance imaging, Sports medicine

Published
2020
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20. Amygdala substructure volumes in Major Depressive Disorder

Author

Darren Roddy, John R. Kelly, Chloë Farrell, Kelly Doolin, Elena Roman, Anurag Nasa, Thomas Frodl, Andrew Harkin, Shane O'Mara, Erik O'Hanlon, and Veronica O'Keane

Subjects
Major Depressive Disorder, Amygdala, Centromedial nucleus, Cortisol awakening response, Hypothalamic-pituitary-adrenal axis, Freesurfer, Computer applications to medicine. Medical informatics, R858-859.7, Neurology. Diseases of the nervous system, RC346-429
Abstract

The role of the amygdala in the experience of emotional states and stress is well established. Connections from the amygdala to the hypothalamus activate the hypothalamic–pituitaryadrenal (HPA) axis and the cortisol response. Previous studies have failed to find consistent whole amygdala volume changes in Major Depressive Disorder (MDD), but differences may exist at the smaller substructural level of the amygdala nuclei. High-resolution T1 and T2-weighted-fluid-attenuated inversion recovery MRIs were compared between 80 patients with MDD and 83 healthy controls (HC) using the automated amygdala substructure module in FreeSurfer 6.0. Volumetric assessments were performed for individual nuclei and three anatomico-functional composite groups of nuclei. Salivary cortisol awakening response (CAR), as a measure of HPA responsivity, was measured in a subset of patients. The right medial nucleus volume was larger in MDD compared to HC (p = 0.002). Increased right-left volume ratios were found in MDD for the whole amygdala (p = 0.004), the laterobasal composite (p = 0.009) and in the central (p = 0.003) and medial (p = 0.014) nuclei. The CAR was not significantly different between MDD and HC. Within the MDD group the left corticoamygdaloid transition area was inversely correlated with the CAR, as measured by area under the curve (AUCg) (p ≤ 0.0001). In conclusion, our study found larger right medial nuclei volumes in MDD compared to HC and relatively increased right compared to left whole and substructure volume ratios in MDD. The results suggest that amygdala substructure volumes may be involved in the pathophysiology of depression.

Published
2021
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24. Hippocampal and Amygdalar Volume Changes in Major Depressive Disorder: A Targeted Review and Focus on Stress

Author

Mark Nolan, Elena Roman, Anurag Nasa, Kirk J. Levins, Erik O’Hanlon, Veronica O’Keane, and Darren Willian Roddy

Subjects
Psychiatry, RC435-571
Abstract

Medial temporal lobe structures have long been implicated in the pathogenesis of major depressive disorder. Although findings of smaller hippocampal and amygdalar volumes are common, inconsistencies remain in the literature. In this targeted review, we examine recent and significant neuroimaging papers examining the volumes of these structures in major depressive disorder. A targeted PubMed/Google Scholar search was undertaken focusing on volumetric neuroimaging studies of the hippocampus and amygdala in major depressive disorder. Where possible, mean volumes and accompanying standard deviations were extracted allowing computation of Cohen’s d s effect sizes. Although not a meta-analysis, this allows a broad comparison of volume changes across studies. Thirty-nine studies in total were assessed. Hippocampal substructures and amygdale substructures were investigated in 11 and 2 studies, respectively. The hippocampus was more consistently smaller than the amygdala across studies, which is reflected in the larger cumulative difference in volume found with the Cohen’s d s calculations. The left and right hippocampi were, respectively, 92% and 91.3% of the volume found in controls, and the left and right amygdalae were, respectively, 94.8% and 92.6% of the volume of controls across all included studies. The role of stress in temporal lobe structure volume reduction in major depressive disorder is discussed.

Published
2020
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25. A comprehensive regional neurochemical theory in depression: a protocol for the systematic review and meta-analysis of 1H-MRS studies in major depressive disorder

Author

Thomas Drago, Patrick W O’Regan, Ivan Welaratne, Shane Rooney, Aoife O’Callaghan, Marissa Malkit, Elena Roman, Kirk J Levins, Lauren Alexander, Denis Barry, Erik O’Hanlon, Veronica O’Keane, and Darren William Roddy

Subjects
Magnetic resonance spectroscopy, Major depressive disorder, Systematic review, Meta-analysis, Metabolite variation, Medicine
Abstract

Abstract Background Magnetic resonance spectroscopy (MRS) is a non-invasive analytical technique that investigates the presence and concentrations of brain metabolites. In the context of major depressive disorder (MDD), MRS has revealed regional biochemical changes in GABA, glutamate, and choline across different brain compartments. Technical and methodological advances in MRS data acquisition, in particular proton-based 1H-MRS, have resulted in a significant increase in the incidence of reports utilizing the technique for psychiatric disorder research and diagnosis. The most recent comprehensive meta-analysis reviewing MRS in MDD stems from 2006. Using contemporary systemic reviews and meta-analysis, the aim is to first test a neurochemical circuit-based theory of depression and then to determine if clinical scores relate to metabolite concentrations before and during treatment. Methods Region-specific metabolite changes in MDD will be assessed by systematic review following the Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA). Inclusion criteria will include participant age (18 to 65), English language studies, known regions of interest, and detailed documentation of 1H-MRS procedures. Reported brain regions will be standardized according neuroanatomical expertise allowing increased power of the meta-analysis. Regions of interest will initially include the hippocampus, thalamus, prefrontal cortex, anterior and posterior cingulate gyri, parietal lobe, and basal ganglia. Exclusion criteria will include comorbid psychiatric illness and drug use. Two independent reviewers will undertake all data extraction, while a third reviewer will check for reviewer discrepancies. Statistical analysis will be performed using STATA supplemented by Metan software and SPSS. Discussion This data will shed new light on the biochemical basis of depression in different brain regions, thereby highlighting the potential of MRS in identifying biomarkers and generating models of MDD and treatment response. Systematic review registration PROSPERO CRD42018091494

Published
2018
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26. Leydig Cell Hyperplasia Mimicking a Testicular Tumour in a Patient with Klinefelter Syndrome

Author

Christine Newman, Stephen Connolly, Owen MacEneaney, Conor O'Keane, and Siobhan E McQuaid

Subjects
Leydig cell hyperplasia, Klinefelter syndrome, Medicine
Abstract

Background: Klinefelter syndrome (KS) is the most common sex-chromosomal disorder in males. Frequently under-recognized, it occurs in 1 in 500–600 male births. It is caused by the inheritance of at least one additional X chromosome from either parent. Patients often have uncommon or atypical malignancies. Patient: We describe the case of a 35-year-old man with 47XXY KS and previous cryptorchidism, presenting with a painful testicular mass. Histology confirmed Leydig cell hyperplasia. Discussion: Cryptorchidism is an established risk factor for testicular tumours and occurs six times more commonly in KS than in the general population. Despite this, large epidemiological studies have shown a reduced burden of testicular cancer in these patients. The presentation of a hypoechoic lesion on ultrasound will prompt consideration of testicular tumours, however orchalgia represents an atypical presentation. In patients with KS, Leydig cell hyperplasia is a much more common entity and should be considered early in the differential diagnosis.

Published
2019
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27. Cornu Ammonis Changes Are at the Core of Hippocampal Pathology in Depression

Author

Darren Roddy and Veronica O’Keane

Subjects
Psychiatry, RC435-571
Abstract

Commentary on: Roddy DW, Farrell C, Doolin K, Roman E, Tozzi L, Frodl T, O'Keane V, O'Hanlon E. The Hippocampus in Depression: More Than the Sum of Its Parts? Advanced Hippocampal Substructure Segmentation in Depression. Biol Psychiatry. 2019 Mar 15;85(6):487-497. doi: 10.1016/j.biopsych.2018.08.021. Epub 2018 Sep 6. PubMed PMID: 30528746. The hippocampus is a key cognitive hub implicated in major depressive disorder. However, major depressive disorder neuroimaging studies have used inconsistent anatomical hippocampal definitions to estimate hippocampal volumes, leading to some heterogeneity in findings. In a recent paper, we used a novel reassembly of automated hippocampal substructures (composites) to build alternative anatomical hippocampal definitions and used these to investigate differences in a well-defined cohort of major depressive disorder patients and healthy controls. We found that the most significant differences between major depressive disorder and healthy controls were localized to the core cornu ammonis (CA) regions of the hippocampus. The CA2–4 regions were smaller in first episode major depressive disorder, whereas more widespread differences were found in recurrent/chronic major depressive disorder, suggestive of a potential disease process in major depressive disorder. In this commentary, we also show how new hippocampal composites to investigate sections of the hippocampal circuitry demonstrate that differences in major depressive disorder occur across the input, middle and output circuit nodes of the hippocampal core. Hippocampal pathology localized across the core hippocampal CA circuity may account for the diverse and wide-ranging symptoms often experienced in depression.

Published
2019
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28. Papez’s Forgotten Tract: 80 Years of Unreconciled Findings Concerning the Thalamocingulate Tract

Author

Joshua Weininger, Elena Roman, Paul Tierney, Denis Barry, Hugh Gallagher, Paul Murphy, Kirk J. Levins, Veronica O’Keane, Erik O’Hanlon, and Darren W. Roddy

Subjects
thalamocingulate tract, thalamus, cingulum, Papez circuit, cingulate cortex, anterior thalamic radiation, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571, Human anatomy, QM1-695
Abstract

The thalamocingulate tract is a key component of the Papez circuit that connects the anterior thalamic nucleus (ATN) to the cingulum bundle. While the other white matter connections, consisting of the fornix, cingulum bundle and mammillothalamic tract, were well defined in Papez’s original 1937 paper, the anatomy of the thalamocingulate pathway was mentioned only in passing. Subsequent research has been unable to clarify the precise anatomical trajectory of this tract. In particular, the site of thalamocingulate tract interactions with the cingulum bundle have been inconsistently reported. This review aims to synthesize research on this least studied component of the Papez circuit. A systemic approach to reviewing historical anatomical dissection and neuronal tracing studies as well as contemporary diffusion magnetic resonance imaging studies of the thalamocingulate tract was undertaken across species. We found that although inconsistent, prior research broadly encompasses two differing descriptions of how the ATN interfaces with the cingulum after passing laterally through the anterior limb of the internal capsule. The first group of studies show that the pathway turns medially and rostrally and passes to the anterior cingulate region (Brodmann areas 24, 33, and 32) only. A second group suggests that the thalamocingulate tract interfaces with both the anterior and posterior cingulate (Brodmann areas 23 and 31) and retrosplenial region (Brodmann area 29). We discuss potential reasons for these discrepancies such as altering methodologies and species differences. We also discuss how these inconsistencies may be resolved in further research with refinements of terminology for the cingulate cortex and the thalamocingulate tract. Understanding the precise anatomical course of the last remaining unresolved final white matter tract in the Papez circuit may facilitate accurate investigation of the role of the complete Papez circuit in emotion and memory.

Published
2019
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30. Awakening Neuropsychiatric Research Into the Stria Medullaris: Development of a Diffusion-Weighted Imaging Tractography Protocol of This Key Limbic Structure

Author

Darren W. Roddy, Elena Roman, Shane Rooney, Sinaoife Andrews, Chloe Farrell, Kelly Doolin, Kirk J. Levins, Leonardo Tozzi, Paul Tierney, Denis Barry, Thomas Frodl, Veronica O’Keane, and Erik O’Hanlon

Subjects
stria medullaris, DTI, tractography, CSD, habenula, depression, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571, Human anatomy, QM1-695
Abstract

The Stria medullaris (SM) Thalami is a discrete white matter tract that directly connects frontolimbic areas to the habenula, allowing the forebrain to influence midbrain monoaminergic output. Habenular dysfunction has been shown in various neuropsychiatric conditions. However, there exists a paucity of research into the habenula’s principal afferent tract, the SM. Diffusion-weighted tractography may provide insights into the properties of the SM in vivo, opening up investigation of this tract in conditions of monoamine dysregulation such as depression, schizophrenia, addiction and pain. We present a reliable method for reconstructing the SM using diffusion-weighted imaging, and examine the effects of age and gender on tract diffusion metrics. We also investigate reproducibility of the method through inter-rater comparisons. In consultation with neuroanatomists, a Boolean logic gate protocol was developed for use in ExploreDTI to extract the SM from constrained spherical deconvolution based whole brain tractography. Particular emphasis was placed on the reproducibility of the tract, attention to crossing white matter tract proximity and anatomical consistency of anterior and posterior boundaries. The anterior commissure, pineal gland and mid point of the thalamus were defined as anatomical fixed points used for reconstruction. Fifty subjects were scanned using High Angular Resolution Diffusion Imaging (HARDI; 61 directions, b-value 1500 mm3). Following constrained spherical deconvolution whole brain tractography, two independent raters isolated the SM. Each output was checked, examined and cleaned for extraneous streamlines inconsistent with known anatomy of the tract by the rater and a neuroanatomist. A second neuroanatomist assessed tracts for face validity. The SM was reconstructed with excellent inter-rater reliability for dimensions and diffusion metrics. Gender had no effect on the dimensions or diffusion metrics, however radial diffusivity (RD) showed a positive correlation with age. Reliable identification and quantification of diffusion metrics of the SM invites further exploration of this key habenula linked structure in neuropsychiatric disorders such as depression, anxiety, chronic pain and addiction. The accurate anatomical localization of the SM may also aid preoperative stereotactic localization of the tract for deep brain stimulation (DBS) treatment.

Published
2018
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32. How does the brain deal with cumulative stress? A review with focus on developmental stress, HPA axis function and hippocampal structure in humans

Author

Thomas Frodl and Veronica O'Keane

Subjects
Major depressive disorder, Cortisol, MRI, Hippocampus, Childhood maltreatment, Dexamethasone suppression test, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571
Abstract

There is evidence that excessive stress exposure of the brain, mediated through the neurotoxic effects of cortisol and possibly neuroinflammation, causes damage to brain structure and function: the glucocorticoid cascade hypothesis. Functional changes of hypothalamic–pituitary–adrenal (HPA) axis as well as alterations in brain structures like the hippocampus have been consistently reported in major depression. However, there has not been a lot of emphasis on bringing findings from studies on early childhood stress, HPA axis functioning and hippocampal imaging together. This is the subject for this systematic review of the literature on how developmental stress, specifically childhood maltreatment, may impact on HPA axis function and hippocampal structure. We will also review the literature on the relationship between HPA axis function and hippocampal volume in healthy, depressed and other disease states. There is evidence that prenatal stress and childhood maltreatment is associated with an abnormally developing HPA system, as well as hippocampal volume reduction. Smaller hippocampal volumes are associated with increased cortisol secretion during the day. We conclude that a model integrating childhood maltreatment, cortisol abnormalities and hippocampal volume may need to take other factors into account, such as temperament, genetics or the presence of depression; to provide a cohesive explanation of all the findings. Finally, we have to conclude that the cascade hypothesis, mainly based on preclinical studies, has not been translated enough into humans. While there is evidence that early life maltreatment results in structural hippocampal changes and these are in turn more prominent in subjects with higher continuous cortisol secretion it is less clear which role early life maltreatment plays in HPA axis alteration.

Published
2013
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35. Diurnal Hypothalamic-Pituitary-Adrenal Axis Measures and Inflammatory Marker Correlates in Major Depressive Disorder

Author

Kelly Doolin, Chloe Farrell, Leonardo Tozzi, Andrew Harkin, Thomas Frodl, and Veronica O’Keane

Subjects
major depressive disorder, hypothalamic-pituitary-adrenal axis, immune system, cortisol awakening response, inflammation, Biology (General), QH301-705.5, Chemistry, QD1-999
Abstract

Dysregulation of the hypothalamic-pituitary-adrenal (HPA) axis and inflammatory systems is a consistent finding in patients with Major Depressive Disorder (MDD). Cortisol is often assessed by measurement of the cortisol awakening response (CAR) and/or diurnal cortisol levels. Some methods of cortisol measurement overestimate cortisol concentration due to detection of other glucocorticoids including the relatively inert cortisone, therefore this study aimed to assess the presence of both cortisol and cortisone, and the cortisol-cortisone catalyzing enzyme 11β-hydroxysteroiddehydrogenase type 1 (11β-HSD1), in depressed patients and controls. Because the HPA axis is known to regulate the body’s immune system, relationships between measures of cytokines and cortisol were also assessed. Saliva samples were collected from 57 MDD patients and 40 healthy controls at five post-wakening time points (0, +30, +60, +720 and +750 min). Glucocorticoid concentrations were measured by liquid chromatography mass spectrometry. Whole blood mRNA expression of several inflammatory markers was measured by quantitative polymerase chain reaction. This study replicated the common finding of elevated morning cortisol and reduced CAR reactivity in MDD and found no differences in cortisone or 11β-HSD1 mRNA measures. There was a negative association between interleukin 1-β (IL-1β) mRNA and morning cortisol reactivity within the depressed group, indicating that dysregulation of the HPA axis and immune system may be interconnected.

Published
2017
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37. Irish society of gastroenterology: Proceedings of meeting held friday 20th and saturday 21st november 1998

Author

Curry, M. P., Norris, S., Hegarty, J. E., Smith, F., Nolan, N., Golden-Mason, L., O’Farrelly, C., Walsh, K. M., Fletcher, A., MacSween, R. N. M., Morris, A. J., Bohan, A., Nolan, N., Hegarty, J. E., Ryan, E., Flanagan, A-M., Martinez-Dalmau, P., Crowe, J., O’Farrelly, C., Golden-Mason, L., Curry, M. P., Kelly, J., Traynor, O., Hegarty, J. E., Mathias, J., McCormick, P. A., McEntee, G., Hegarty, J., Traynor, O., Barrett, S., O’Keane, J. C., Crowe, J., Shah, A. A., Berry, M., Thjodleifsson, B., Bjarnason, I., Gudjohnsson, H., Oddson, E., Fitzgerald, D. J., Kay, E., Price, A., Murray, F. E., Carton, E., Mulligan, E. D., Caldwell, M. T. P., Rana, D., Ryan, B., Mahmud, N., Keeling, N., Tanner, W. A., Keane, F. B. V., McDonald, G., Reynolds, J. V., Mahmood, Z., Rathore, O., Ellis, I., Byrne, P., Mahmud, N., Keeling, P. W. N., Khan, I., McManus, K., Anikin, V., Mills, M., McGuigan, J., Taylor, C., Winter, D. C., O’Sullivan, G. C., Harvey, B. J., Bennett, M. W., O’Connell, J., O’Sullivan, G. C., Collins, J. K., Shanahan, F., Wieneke, P., O’Leary, C., Healy, M., O’Halloran, T., Barry, R., Cronin, C. C., O’Regan, P., Shanahan, F., Bennett, M. W., O’Connell, J., O’Sullivan, G. C., Collins, J. K., Shanahan, F., O’Grady, H., Grant, D., Sheahan, K., Hyland, J. M. P., O’Donoghue, D. P., Murphy, J., Lee, G., Madden, M., Kelly, J., Collins, J. K., Shanahan, P., Sullivan, G. O., Shima, H., Basisht, R., Ohshiro, K., Puri, P., Goh, J., MacMathuna, P., Baird, A., Godson, C., Brady, H. R., Petasis, N. A., Fokin, V. V., O’Keane, J. C., McCormack, G., McCormick, P. A., Hegarty, J. E., O’Donoghue, D. P., Hyland, J. M. P., Khosraviani, K., Weir, H. P., Williamson, K., Hamilton, P., Moorehead, R. J., Mcllmoyle, J., Watson, R. G. P., Collins, J. S. A., Tham, T. C. K., Doyle, R. M., Molony, C., Fitzpatrick, D., Coakley, D., Walsh, J. B., Kelleher, D., Devitt, E., Keane, C., Walsh, C., Bennett, M. W., O’Connell, J., O’Sullivan, G. C., Collins, J. K., Shanahan, F., Murray, K. P., Kaufman, H. S., Shin, J. H., Pitt, H. A., Johnston, S. D., Watson, R. G. P., McMillan, S. A., Larkin, C. J., Sloan, J. M., Watson, R. G. P., Ardill, J. E. S., Collins, J. S., Buchanan, K. D., Larkin, C. J., Curry, W. J., Watson, R. G. P., Johnston, C. F., Ardill, J. E. S., Buchanan, K. D., Larkin, C. J., Curry, W., Johnston, C., Sloan, J., Watson, R. G. P., Ardill, J., Collins, J. S., Buchanan, K. D., Larkin, C. J., Curry, W., Johnston, C., Sloan, J., Watson, R. G. P., Ardill, J., Collins, J. S., Buchanan, K. D., Larkin, C. J., Irvine, R., Gibson, L., Tham, T. C. K., Creedon, G., Mabruk, M., Leader, M., O’Grady, T., Murphy, M., Kay, E., Shah, A. A., Harhen, B., Fitzgerald, D. J., Murray, F. E., Hickey, A., Gannon, N., O’Boyle, C., Byrne, R., Smith, M., Murray, F., Byrne, M. F., Harhen, B., Fitzgerald, D. J., Murray, F. E., Quinlan, J., Delaney, C. P., O’Grady, H., Varadarajan, R., O’Donoghue, D. P., Hyland, J. M., MacEneaney, P. M., Skehan, S. J., Curry, M., Gibney, R. G., McCormick, P. A., Malone, D. E., Kealy, S., MacEneaney, P. M., Dodd, J., Murrary, R., Donoghue, D. P., Keating, D., Gibney, R. G., Malone, D. E., Hashim, Z., Donnellan, J., O’Connor, Y., Kearns, M., Stevens, F. M., Sookhai, S., Wang, J. H., Neary, P., McCourt, M., O’Connell, D., Redmond, H. P., Khosraviani, K., McAteer, E., Campbell, W. J., Mackle, E. J., Smyth, C., McKiernan, S., Lawlor, M., Pilkington, K., Hagan, R., Kelleher, D., Montague, S., Barry, R., Buckley, M., Morain, C. A. O., Connolly, C., Tierney, S., Gray, J., Lyons, N. D., Delaney, P. V., Grace, P. A., Nemeth, L., O’Briain, D. S., Puri, P., Carton, E., Mulligan, E. D., O’Toole, C., Roddy, D., Keeling, N., Griffin, M., McDonald, G., Hennessy, T. P. J., Reynolds, J. V., O’Keffe, C., O’Donoghue, D., Hegarty, J., McCormick, P. A., Murphy, E., Reynolds, J., Nolan, J. J., Goh, J., Barrett, S., McAndrew, M., Crowe, J., O’Keane, J. C., Clarke, G., Stewart, S., McKiernan, S., Cockram, A., O’Keane, J. C., Kelleher, D., Crowe, J., Coughlan, B., Sheehan, J., Hickey, A., Crowe, J., Lang, E. E., Caldwell, M. T. P., Tanner, W. A., McNamara, D., Hamilton, H., Beattie, S., Montague, S., O’Morain, C., Windle, H. J., Kelleher, D., Heaney, A., Collins, J. S. A., Tham, T. C. K., Chan, W. S., Mitchell, R. M. S., Collins, J. S. A., Watson, R. G. P., O’Leary, C., Wieneke, P., Feighery, L., Quane, K., Molloy, M., Shanahan, F., Feighery, C., Cronin, C. C., Golden-Mason, L., Curry, M. P., Traynor, O., McEntee, G., Kelly, J., Hegarty, J. E., Farrelly, C. O., Egan, B. M., Barry, M. K., Grant, D. C., O’Donoghue, D., Hegarty, J., Traynor, O., Hyland, J. M. P., Barry, P., Casey, P., Laffoy, M., Tracey, J., McCormick, P. A., Goode, T., O’Connell, J., Hopkins, A., Baird, A. W., O’Sullivan, G. C., Collins, J. K., Shanahan, F., O’Leary, C., Kingston, M., Blackwell, M., Wieneke, P., Cronin, C. C., O’Regan, P. F., Shanahan, F., Maher, L. J., Skelly, M. M., Godson, C., Brady, H. R., and Baird, A. W.

Published
1998
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38. Irish society of gastroenterology: Proceedings of meeting held Friday 12th and Saturday 13th June, 1998

Author

Ryan, B. M., McKiernan, S., Keeling, P. W. N., Byrne, P. J., Quill, R., McCallion, K., Mitchell, R. M. S., Watson, R. G. P., Collins, J. S. A., Gardiner, K. R., Winter, D. C., O’Sullivan, G. C., Taylor, C. T., Fanning, N. F., Redmond, H. P., O’Donoghue, D. P., Baird, A. W., Harvey, B. J., Brannigan, A. E., O’Connell, P. R., Regan, M. C., Fitzpatrick, J. M., Watson, R. W. G., Lemass, H., Ryan, E., MacMathuna, P., Crowe, J., O’Keane, J. C., Goh, J., MacMathuna, P., Baird, A., Maher, L., Godson, C., Brady, H. R., Petasis, N. A., Fokin, V. V., O’Keane, J. C., Barry, M. K., Grant, D. C., Sheahan, K., O’Donoghue, D. P., Hyland, J. M. P., Sheehan, K. M., Sheahan, K., O’Donoghue, D. P., Fitzgerald, D. J., Murray, F. E., Heaney, A., Collins, J. S. A., Bamford, K. B., Watson, R. G. P., McFarland, R. J., Tham, T. C. K., McNamara, D., Franelli, S., Whelan, H., Hamilton, H., Beattie, S., O’Morain, C., Ryan, B. M., Keeling, P. W. N., Brennan, E. G., O’Hare, N., McDermott, R., Byrne, P. J., McDougall, N. I., Collins, J. S. A., Gieeson, C. M., Russell, S. E. H., Sloan, J. M., Morrisey, D., Murphy, L., Kiely, B., Fitzgerald, G., Daly, C., O’Sullivan, G., Shanahan, F., Collins, J. K., Marteau, P., Johnston, S. D., Watson, R. G. P., Coates, C., Feighery, C., O’Keeffe, J., Whelan, A., Lynch, S., Weir, D. G., Abuzakouk, M., Feighery, C., Barnes, L., O’Gorman, N., McKenna, M., Freaney, R., Young, M., Gaines, S., Brady, D., Drudy, D., O’Farrelly, C., Gilleece, A., Fenelon, L., McPartlin, J., Goh, J., MacMathuna, P., Baird, A., Godson, C., Brady, H. R., Petasis, N. A., Fokin, V. V., Hopkins, A. M., Myers, A., Moynagh, P., Baird, A. W., O’Donoghue, D. P., Kirby, J. M., Tham, T. C. K., Allen, M. J., Best, B., Calvert, H., Kirk, S., McKelvey, S. T. D., Moorehead, R. J., Varghese, J. C., Sookhai, S., Murray, F. E., Walsh, T., Osborne, H., Broe, P., Lee, M. J., Moriarty, D., Baird, A. W., Watson, R. W. G., Brannigan, A. E., Coffey, R., Murphy, E., Fitzpatrick, J. M., Shah, A. A., Murray, F. E., Murray, E., Thjodleifsson, B., Bjarnason, I., Fitzgerald, D. J., Sheehan, K. M., Murray, E., Shah, A. A., Murray, F. E., Thjodleifsson, B., Bjarnason, I., Fitzgerald, D. J., Montague, S., McNamara, D., Forkin, C., O’Morain, C., O’Toole, G. C., Grant, D. C., Barry, M. K., Sheahan, K., O’Donoghue, D. P., Hyland, J. M. P., Gallagher, C. M., Grant, D. C., Connell, P., Barry, M. K., Traynor, O., Hyland, J. M. P., Barry, M. K., Grant, D. C., Sheahan, K., O’Donoghue, D. P., Hyland, J. M. P., Ling, T. C., Johnston, B., Byrne, M. F., Farrell, M. A., Varghese, J. C., Lee, M. J., Murray, F. E., Goulding, C. A., Albloushi, S. S., O’Connell, P., Murray, F. E., Graham, L. E., Robinson, T. J., Graham, L. E., Robinson, T. J., Jabeen, T., Cannon, B., Jenkins, D., Whelton, M. J., Bohra, S., Cannon, B., Whelton, M. J., Keohane, C., Duggan, M., Bohra, S., Cannon, B., Whelton, M. J., Siddheshwar, R. K., Wilson, R. G., Hainsworth, P. J., Campbell, F. C., Kelly, S. B., Kirby, J. M., Tham, T. C. K., Best, B., Calvert, H., Moorehead, R. J., Kirk, S., Heaney, A., Collins, J. S. A., Watson, R. G. P., Heaney, A., Collins, J. S. A., Watson, R. G. P., Bamford, K. B., McFarland, R. J., Tham, T. C. K., Egan, B. M., Grant, D. C., Barry, M. K., Traynor, O., Hyland, J. M. P., Simutowe, C., McNamara, D. A., Collins, N., Walsh, T. N., Mukherjee, A., Scott, M., Pohl, C., Duggan, E., Wasi, M., Sarkar, A., Donnell, L. O., Eustace, P. W., Johnston, J. G., Waldron, R., Barrett, S., Ryan, E., MacMathuna, P., Crowe, J., Callagy, G., Keane, J. C. O., Coughlan, B., Crowe, J., Sheehan, J., Hickey, A., Carr, A., Kell, M. R., Lynch, M., Ryan, D., Winter, D. C., Rajpal, P., Kirwan, W. O., Redmond, H. P., Larkin, C. J., Sloan, J. M., Watson, R. G. P., Ardill, J. E. S., Collins, J. S. A., Buchanan, K. D., Lim, P. L., Gibbons, M., Crawford, E. J., Johnston, B. T., Mitchell, R. M. S., Watson, R. G. P., Gardiner, K. R., Collins, J. S. A., McCallion, K., Mitchell, R. M. S., Collins, J. S. A., Watson, R. G. P., McCallion, K., Gardiner, K. R., McCallion, K., Gardiner, K. R., Mitchell, R. M. S., Watson, R. G. P., Collins, J. S. A., Rodgers, C., Johnston, S., Watson, R. G. P., Crone, B. M., Love, A. H. G., Feighery, L., Feighery, C., Jackson, J., Abuzakouk, M., Lynch, S., Weir, D. G., Yassin, M. M. I., Harkin, D. W., Barros D’sa, A. A. B., Parks, T. G., Curry, M. P., Hegarty, J. E., Golden-Mason, L., O’Farrelly, C., Hannigan, E., and Parfrey, N.

Published
1998
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39. Irish society of gastroenterology: Proceedings of Winter Meeting held Friday 21st and Saturday 22nd November, 1997

Author

Clarke, G., Ryan, E., O’Keane, J. C., Crowe, J., McMathuna, P., Moriarty, D., Ettarh, R., Sheahan, K., Hyland, J., O’Donoghue, D. P., Baird, A. W., Clarke, G., Ryan, E., Gormley, G., Keane, J. C. O., Crowe, J., MacMathuna, P., Wang, J. H., Wu, Q. D., Redmond, H. P., Condron, C., Bouchier-Hayes, D., Nally, K., Newton, F., O’Connell, J., O’Sullivan, G. C., Morgan, J., Collins, J. K., Shanahan, F., Goode, C., O’Connell, J., O’Sullivan, G. C., Collins, J. K., Shanahan, F., Winter, D. C., Taylor, C. T., Skelly, M. M., O’Donoghue, D. P., O’Sullivan, G. C., Baird, A. W., Harvey, B. J., Varghese, J. C., Farrell, M. A., McGrath, F. P., Murray, F. E., Osborne, H., Lee, M. J., Ryan, E., Sullivan, A., O’Keane, J. C., Crowe, J., Ryan, A. E., O’Keane, J. C., Crowe, J., Donovan, A. N., McCormick, P. A., Kenny, B., Somers, S., Bohan, A., Gibney, R. G., Marcaccio, M., Malone, D. E., Doyle, M., Delaney, C. P., Gorey, T. F., McEntee, G. P., O’Sullivan, G. C., Clarke, A., Stuart, R., Kelly, J., Kiely, M. D., Collins, J. K., Shanahan, F., O’Sullivan, M., Lovett, E., Mahmud, N., Kelleher, D., O’Morain, C. A., Larkin, C. J., Watson, R. G. P., Sloan, J. M., Ardill, J. E. S., Johnston, C. F., Buchanan, K. D., Heaney, A., Collins, J. S. A., Watson, G. R. P., Kalin, R. M., Heaney, A., Collins, J. S. A., Tham, T. C. K., Watson, R. G. P., McFarland, R. J., Bamford, K. B., Cróinín, T. Ó, Clyne, M., Drumm, B., Rowland, M., Kumar, D., O’Connor, P., Daly, L. E., Drumm, B., O’Toole, D. L., Long, A., Murphy, A. M., O’Neill, L., Weir, D. G., Kelleher, D., Heaney, A., Collins, J. S. A., Watson, R. G. P., Hopkins, A. M., Moynagh, P., O’Donoghue, D. P., Baird, A. W., Brennan, C., Harmey, J., Stapleton, P. P., Redmond, H. P., Bouchier-Hayes, D., Rasheed, A. M., Chen, G., Kelly, C., Bouchier-Hayes, D. J., Leahy, A., Gallagher, M., Grace, A., Xin, Y., Leader, M., Kay, E., Whelan, A., Pattison, U., Willoughby, R., Wallace, E., Weir, D., Feighery, C., Bennett, M. W., O’Connell, J., O’Sullivan, G. C., Brady, C., Roche, D., Collins, J. K., Shanahan, F., Mahmud, N., Molloy, A., McPartlin, J., Scott, J. M., Weir, D. G., Acheson, A. G., Lee, J., Khosraviani, K., Irwin, S. T., McDaid, J., McCormick, P. A., Docherty, J. R., O’Grady, A., Kay, E., Mabruk, M., Grace, A., Leader, M., Lee, J., Acheson, A. G., Irwin, S. T., Larkin, C. J., Johnston, C., Curry, W., Ardill, J., Cunningham, R., Buchanan, K. D., Watson, R. G. P., McDougall, N. I., Coyle, P. V., Callender, M. E., Ouinn, A. M., Warner, R., Stevens, F. M., Chakravarthi, P. I. S., Kearns, M., Bourke, M., Hassan, A., McWeeney, J., Stevens, F. M., McCarthy, C. F., Casey, M., O’Donoghue, J., Eustace-Ryan, A. M., O’Regan, P., Feighery, L., Jackson, J., Cronin, N., Shanahan, F., Quane, K., Feighery, C., Mulligan, E. D., Purcell, T., Dunne, B., Griffin, M., Noonan, N., Hollywood, D., Keeling, N., Reynolds, J. V., Hennessy, T. P. J., Mulligan, E. D., Purcell, T., Dunne, B., Griffin, M., Noonan, N., Hollywood, D., Keeling, N., Reynolds, J. V., Hennessy, T. P. J., Mulligan, E. D., Purcell, T., Dunne, B., Griffin, M., Noonan, N., Hollywood, D., Keeling, N., Reynolds, J. V., Hennessy, T. P. J., Mulligan, E. D., Purcell, T., Dunne, B., Griffin, M., Noonan, N., Hollywood, D., Keeling, N., Reynolds, J. V., Hennessy, T. P. J., O’Sulhvan, M., Harman, I., Breslin, N. P., Clayton, N., O’Morain, C. A., Hogan, S., Donovan, B., Hayes, D., Kiely, M., Eustace-Ryan, A. M., O’Regan, P., Goulding, C. A., Albloushi, S. S., O’Connor, J., Courtney, M. G., Murray, F. E., Albloushi, S. S., Goulding, C. A., Kay, E., Royston, D., Leader, M., Courtney, M. G., Murray, F. E., Albloushi, S. S., Kay, E., Goulding, C. A., Grace, A., O’Connor, J., Shattock, A. G., Courtney, M. G., Murray, F. E., Albloushi, S. S., Stack, A., Kay, E., Goulding, C. A., Carmody, M., Murray, F. E., Courtney, M. G., Barrett, S., Ryan, E., O’Keane, J. C., Crowe, J., Hennigan, A., Delaney, C. P., Young, L., Shields, C. J., O’Keane, C., Gorey, T. F., Fitzpatrick, J. M., Rasheed, A. M., Wang, J. H., Kelly, C., Bouchier-Hayes, D. J., Leahy, A., Doyle, M. M., Stephens, R. B., Daly, P. A., Bennett, M. W., O’Connell, J., O’Sullivan, G. C., Brady, C., Roche, D., Collins, J. K., Shanahan, F., Briggs, G. M., McCrory, D., Briggs, G. M., McCrory, D., O’Neill, S., O’Grady, H., Grant, D. C., Barry, K., Traynor, O., Hyland, J. M. P., O’Toole, G. C., Grant, D. C., Barry, M. K., Hyland, J. M. P., Johnston, S. D., Ritchie, C. M., Robinson, T. J., Johnston, S. D., Kirby, J. M., Mackle, E. M., Robinson, T. J., Haider, N., Aherne, N., McNichol, F., Hamilton, D., Neary, P., Hegarty, S., Connor, J. O., Watson, R. G. K., Drudy, D., Alwan, A., Fenelon, L., O’Farrelly, C., Hyland, J., Byrne, B., Madrigal, L., Carton, J., Collins, C., O’Donoghue, D., O’Farrelly, C., Gannon, N., Hickey, A., O’Boyle, C. A., Byrne, R., Albloushi, S., and Murray, F.

Published
1998
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44. Developmental model of depression applied to prenatal depression: role of present and past life events, past emotional disorders and pregnancy stress.

Author

Jacques Dayan, Christian Creveuil, Michel Dreyfus, Michel Herlicoviez, Jean-Marc Baleyte, and Veronica O'Keane

Subjects
Medicine, Science
Abstract

BackgroundSeveral risk factors for depression during pregnancy have already been established. However, very few studies have conducted a multivariate analysis incorporating both the major predictors of depression in women, in accordance with comprehensive developmental models of depression, and specific stressors associated with the biological and psychosocial state of the mother-to-be.Methodology/principal findingsWe used a cross-sectional cohort design to analyze the associations between prenatal depression and potential risk factors. 693 French-speaking women with singleton pregnancies at 20-28 weeks' gestation were consecutively recruited at Caen University Hospital. Fifty women with missing values were subsequently excluded from the analysis. Depressive symptoms were assessed on the Edinburgh Postnatal Depression Scale. Risk factors were either extracted from the computerized obstetric records or assessed by means of self-administered questionnaires. The associations between prenatal depression and the potential risk factors were assessed using log-binomial regression models to obtain a direct estimate of relative risk (RR). The following factors were found to be significant in the multivariate analysis: level of education (pConclusions/significanceOur study identifies several risk factors that could easily be assessed in clinical practice. It draws attention to the impact of previously delivering a child with a birth defect. The association with childhood adversity warrants further study.

Published
2010
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50. Sylvester o’halloran surgical scientific meeting: Proceedings of meeting held 6th & 7th March 1998 in the Foundation Building, University of Limerick

Author

Relihan, N., McGreal, G., Murray, M., McDermott, E. W., O’Higgins, N. J., Duffy, M. J., McNamara, D. A., Harmey, J., Wang, J. H., Donovan, D., Walsh, T. N., Bouchier-Hayes, D. J., Kay, E., Kelly, J. D., Weir, H. P., Keane, P. F., Johnston, S. R., Williamson, K. E., Hamilton, P. W., McManus, D., Morrin, M., Delaney, P. V., Winter, D. C., Harvey, B. J., Geibel, J. P., O’Sullivan, G. C., Delaney, C. P., Coffey, R., Gorey, T. F., Fitzpatrick, J. M., Fanning, N. F., Kirwan, W., Cotter, T., Bouchier-Hayes, D., Redmond, H. P., McNamara, D. A., Pidgeon, G., Harmey, J., Walsh, T. N., Bouchier-Hayes, D. J., Redmond, H. P., Fennessy, F., Wang, J. H., Kelly, C., Bouchier-Hayes, D., Delaney, C. P., Flavin, R., Coffey, R., Gorey, T. F., Fitzpatrick, J. M., Rasheed, A. M., Wang, J. H., Kelly, C., Bouchier-Hayes, D. J., Leahy, A., Lang, E. E., Caldwell, M. T. P., Tanner, W. A., Kiely, P. D., O’Reilly, M., Tierney, S., Barry, M., Delaney, P. V., Drumm, J., Grace, P. A., Gallagher, C. M., Grant, D. C., Connell, P., Barry, M. K., Traynor, O., Hyland, J. M. P., O’Sullivan, M. J., Evoy, D., Redmond, H. P., Kirwan, W. O., Cannon, B., Kenny-Walshe, L., Whelton, M. J., O’Grady, H., O’Neill, S., Grant, D. C., Barry, M. K., Traynor, O., Hyland, J. M., Teh, S. H., O’Ceallaigh, S., O’Donohoe, M. K., Tanner, W. A., Keane, F. B., O’Toole, G. C., Grant, D. C., Barry, M. K., Hyland, J. M. P., Calleary, J., Basso, L., Amjad, S. B., Khan, Z., McMullin, L., Joyce, W. P., Balfe, P. J., Caldwell, M. T., Keane, F. B., Tanner, W. A., Teahan, S., Al-Brekeit, K., Tierney, S., Rasheed, A., Bouchier-Hayes, D., Leahy, A., O’Neill, S., Delaney, C. P., Gorey, T. F., Fitzpatrick, J. M., Cullen, A., O’Keane, C., Fennessy, F., Kelly, C., Bouchier-Hayes, D., Fennessy, F., Wang, J. H., Kelly, C., Bouchier-Hayes, D. J., Winter, D. C., MacFarlane, J., Harvey, B. J., O’Sullivan, G. C., Walsh, M., McGloughlin, T., Grace, P., Colgan, D., Madhavan, P., Sultan, S., Colgan, M. P., Moore, D., Shanik, G., McEniff, N., Molloy, M., Eguare, E., Fiuza, C., Grace, P., Burke, P., Maher, R., Creamer, M., Cronin, C. J., Sigurdsso, H. H., Kim, W., Linklater, G., Cross, K. S., Simpson, W. G., Shaw, J. A. M., Pearson, D. W. M., Fitzgerald, P., Quinn, P., Tierney, S., Bouchier-Hayes, D., Brady, C. M., Shah, S. M. A., Ehtisham, M., Khan, M. S., Flood, H. D., Loubani, M., Sweeney, K., Lenehan, B., Lynch, V., Joy, A., McGreal, G., Reidy, D., Mahalingam, K., Cashman, W., Mulligan, E. D., Purcell, T., Dunne, B., Griffin, M., Noonan, N., Hollywood, D., Keeling, N., Reynolds, J. V., Hennessy, T. P. J., O’Halloran, D., McGreal, G., McDermott, E. W., O’Higgins, N. J., Neary, P., Hamilton, D., Haider, N., Aherne, N., Watson, R. G. K., Walsh, D., Murphy, M., Joyce, M., Johnston, S., Clinton, O., Given, H. F., Brannigan, A., O’Donohoe, M., Donohoe, J., Corrigan, T., Bresnihan, M., O’Donohoe, M. K., Feeley, T. M., Sultan, S., Madhavan, P., Colgan, M. P., Moore, D., Shanik, G., McMonagle, M. P., Quinlan, D., Kelly, D., Hegarty, P. K., Tan, B., Cronin, C., Brady, M. P., Zeeshan, M., McAvinchey, D. J., Aherne, N., Mooney, C., Coyle, D., Haider, N., Hamilton, D., Neary, P., Watson, R. G. K., Khayyat, G., Masterson, E., Thambi-Pillai, T., Farah, K., Delaney, C. P., Codd, M. B., Fitzpatrick, J. M., Gorey, T. F., Barry, M. K., Tsiotos, G. G., Johnson, C. D., Sarr, M. G., Kell, M. R., Lynch, M., Ryan, D., O’Donovan, A., Winter, D. C., Redmond, H. P., Delaney, C. P., Cassidy, M., Doyle, M., Fulton, G., O’Connell, P. R., Kingston, R., Dillon, M., Barry, M., Tierney, S., Grace, P. A., McGreal, G., Lenehan, B., Murray, M., McDermott, E., O’Higgins, N., Kell, M. R., O’Sullivan, R. G., Tan, B., and O’Donnell, J. A.

Published
1998
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