Your search keyword '"Hernandez-Guillamon M"' showing total 31 results

1. Advancing diagnostic criteria for sporadic cerebral amyloid angiopathy: Study protocol for a multicenter MRI-pathology validation of Boston criteria v2.0

Author

Charidimou, A., Frosch, M.P., Salman, R.A., Baron, J.C., Cordonnier, C., Hernandez-Guillamon, M., Linn, J., Raposo, N., Rodrigues, M., Romero, J.R., Schneider, J.A., Schreiber, S., Smith, E.E., Buchem, M.A. van, Viswanathan, A., Wollenweber, F.A., Werring, D.J., Greenberg, S.M., and Int CAA Assoc

Subjects

Pathology, medicine.medical_specialty, business.industry, diagnosis, diagnosis [Cerebral Amyloid Angiopathy], Reproducibility of Results, medicine.disease, pathology [Cerebral Amyloid Angiopathy], Magnetic Resonance Imaging, Sensitivity and Specificity, diagnostic imaging [Cerebral Amyloid Angiopathy], Neurology, cerebral microbleeds, Medicine, Humans, Cerebral amyloid angiopathy, ddc:610, business, Sporadic cerebral amyloid angiopathy, cortical superficial siderosis

Abstract

Rationale The Boston criteria are used worldwide for the in vivo diagnosis of cerebral amyloid angiopathy and are the basis for clinical decision-making and research in the field. Given substantial advances in cerebral amyloid angiopathy's clinical aspects and MRI biomarkers, we designed a multicenter study within the International cerebral amyloid angiopathy Association aimed at further validating the diagnostic accuracy of the Boston and potentially improving and updating them. Aim We aim to derive and validate an updated “version 2.0” of the Boston criteria across the spectrum of cerebral amyloid angiopathy-related presentations and MRI biomarkers. Sample size estimates Participating centers with suitable available data (see Methods) were identified from existing collaborations and an open invitation to the International Cerebral Amyloid Angiopathy Association emailing list. Our study sample will include: (1) a derivation cohort – Massachusetts General Hospital (MGH), Boston cases from inception to 2012 (∼150 patients); (2) temporal external validation cohort – MGH, Boston cases from 2012 to 2018 (∼100 patients); and (3) geographical external validation cohort – non-Boston cases (∼85 patients). Methods and design Multicenter collaborative study. We will collect and analyze data from patients' age ≥ 50 with any potential sporadic cerebral amyloid angiopathy-related clinical presentations (spontaneous intracerebral hemorrhage, transient focal neurological episodes and cognitive impairment), available brain MRI (“index test”), and histopathologic assessment for cerebral amyloid angiopathy (“reference standard” for diagnosis). Trained raters will assess MRI for all prespecified hemorrhagic and non-hemorrhagic small vessel disease markers of interest, according to validated criteria and a prespecified protocol, masked to clinical and histopathologic features. Brain tissue samples will be rated for cerebral amyloid angiopathy, defined as Vonsattel grade ≥2 for whole brain autopsies and ≥1 for cortical biopsies or hematoma evacuation. Based on our estimated available sample size, we will undertake pre-specified cohort splitting as above. We will: (a) pre-specify variables and statistical cut-offs; (b) examine univariable and multivariable associations; and (c) then assess classification measures (sensitivity, specificity etc.) for each MRI biomarker individually, in relation to the cerebral amyloid angiopathy diagnosis reference standard on neuropathology in a derivation cohort. The MRI biomarkers strongly associated with cerebral amyloid angiopathy diagnosis will be selected for inclusion in provisional (probable and possible cerebral amyloid angiopathy) Boston criteria v2.0 and validated using appropriate metrics and models. Study outcomes Boston criteria v2.0 for clinical cerebral amyloid angiopathy diagnosis. Discussion This work aims to potentially update and improve the diagnostic test accuracy of the Boston criteria for cerebral amyloid angiopathy and to provide wider validation of the criteria in a large sample. We envision that this work will meet the needs of clinicians and investigators and help accelerate progress towards better treatment of cerebral amyloid angiopathy.

Published

2019

2. Impact of blood pressure changes and course on hematoma growth in acute intracerebral hemorrhage

Author

Rodriguez-Luna, D., Piñeiro, S., Rubiera, M., Ribo, M., Coscojuela, P., Pagola, J., Flores, A., Muchada, M., Ibarra, B., Meler, P., Sanjuan, E., Hernandez-Guillamon, M., Alvarez-Sabin, J., Montaner, J., and Molina, C. A.

Published

2013

3. Leukoaraiosis is associated with genes regulating blood-brain barrier homeostasis in ischaemic stroke patients

Author

Fernandez-Cadenas, I., Mendioroz, M., Domingues-Montanari, S., Del Rio-Espinola, A., Delgado, P., Ruiz, A., Hernandez-Guillamon, M., Giralt, D., Chacon, P., Navarro-Sobrino, M., Ribo, M., Molina, C. A., Alvarez-Sabin, J., Rosell, A., and Montaner, J.

Published

2011

4. Characterization of ApoJ-reconstituted high-density lipoprotein (rHDL) nanodisc for the potential treatment of cerebral beta-amyloidosis

Author

Fernandez-de-Retana, S, Cano-Sarabia, M, Marazuela, P, Sanchez-Quesada, JL, Garcia-Leon, A, Montanola, A, Montaner, J, Maspoch, D, and Hernandez-Guillamon, M

Abstract

Cerebral beta-amyloidosis is a major feature of Alzheimer's disease (AD), characterized by the accumulation of beta-amyloid protein (A beta) in the brain. Several studies have implicated lipid/ lipoprotein metabolism in the regulation of beta-amyloidosis. In this regard, HDL (High Density Lipoprotein)-based therapies could ameliorate pathological features associated with AD. As apolipoprotein J (ApoJ) is a natural chaperone that interacts with A beta, avoiding its aggregation and toxicity, in this study we propose to prepare reconstituted rHDL-rApoJ nanoparticles by assembling phospholipids with recombinant human ApoJ (rApoJ). Hence, rHDL particles were prepared using the cholate dialysis method and characterized by N-PAGE, dynamic light scattering, circular dichroism and electron transmission microscopy. The preparation of rHDL particles showed two-sized populations with discoidal shape. Functionally, rHDL-rApoJ maintained the ability to prevent the A beta fibrillization and mediated a higher cholesterol efflux from cultured macrophages. Fluorescently-labelled rHDL-rApoJ nanoparticles were intravenously administrated in mice and their distribution over time was determined using an IVIS Xenogen (R) imager. It was confirmed that rHDL-rApoJ accumulated in the cranial region, especially in old transgenic mice presenting a high cerebral A beta load. In conclusion, we have standardized a reproducible protocol to produce rHDL-rApoJ nanoparticles, which may be potentially considered as a therapeutic option for beta-amyloid-related pathologies.

Published

2017

5. Ultraearly hematoma growth predicts poor outcome after acute intracerebral hemorrhage.

Author

Rodriguez-Luna D, Rubiera M, Ribo M, Coscojuela P, Piñeiro S, Pagola J, Hernandez-Guillamon M, Ibarra B, Romero F, Alvarez-Sabin J, Montaner J, Molina CA, Rodriguez-Luna, D, Rubiera, M, Ribo, M, Coscojuela, P, Piñeiro, S, Pagola, J, Hernandez-Guillamon, M, and Ibarra, B

Published

2011

6. PAI-1 4G/5G Polymorphism is Associated with Brain Vessel Reocclusion After Successful Fibrinolytic Therapy in Ischemic Stroke Patients

Author

Fernandez-Cadenas, I., primary, Del Rio-Espinola, A., additional, Rubiera, M., additional, Mendioroz, M., additional, Domingues-Montanari, S., additional, Cuadrado, E., additional, Hernandez-Guillamon, M., additional, Rosell, A., additional, Ribo, M., additional, Alvarez-Sabin, J., additional, Molina, C. A., additional, and Montaner, J., additional

Published

2010

7. Sodium Bicarbonate Enhances Membrane-bound and Soluble Human Semicarbazide-sensitive Amine Oxidase Activity In Vitro

Author

Hernandez-Guillamon, M., primary, Bolea, I., additional, Sole, M., additional, Boada, M., additional, Tipton, K.F., additional, and Unzeta, M., additional

Published

2007

8. Charge effect of a liposomal delivery system encapsulating simvastatin to treat experimental ischemic stroke in rats

Author

Campos-Martorell M, Cano-Sarabia M, Simats A, Hernández-Guillamon M, Rosell A, Maspoch D, and Montaner J

Subjects

Simvastatin, liposomes, delivery, brain, stroke, rat, Medicine (General), R5-920

Abstract

Mireia Campos-Martorell,1 Mary Cano-Sarabia,2 Alba Simats,1 Mar Hernández-Guillamon,1 Anna Rosell,1 Daniel Maspoch,2,3 Joan Montaner1,4 1Neurovascular Research Laboratory, Institut de Recerca Vall d’Hebron, Universitat Autònoma de Barcelona, Barcelona, 2Catalan Institute of Nanoscience and Nanotechnology (ICN2), CSIC and The Barcelona Institute of Science and Technology, Universitat Autònoma de Barcelona, Barcelona, 3Institució Catalana de Recerca i Estudis Avançats (ICREA), 4Neurovascular Unit, Department of Neurology, Universitat Autònoma de Barcelona, Hospital Vall d’Hebron, Barcelona, Spain Background and aims: Although the beneficial effects of statins on stroke have been widely demonstrated both in experimental studies and in clinical trials, the aim of this study is to prepare and characterize a new liposomal delivery system that encapsulates simvastatin to improve its delivery into the brain. Materials and methods: In order to select the optimal liposome lipid composition with the highest capacity to reach the brain, male Wistar rats were submitted to sham or transitory middle cerebral arterial occlusion (MCAOt) surgery and treated (intravenous [IV]) with fluorescent-labeled liposomes with different net surface charges. Ninety minutes after the administration of liposomes, the brain, blood, liver, lungs, spleen, and kidneys were evaluated ex vivo using the Xenogen IVIS® Spectrum imaging system to detect the load of fluorescent liposomes. In a second substudy, simvastatin was assessed upon reaching the brain, comparing free and encapsulated simvastatin (IV) administration. For this purpose, simvastatin levels in brain homogenates from sham or MCAOt rats at 2 hours or 4 hours after receiving the treatment were detected through ultra-high-protein liquid chromatography. Results: Whereas positively charged liposomes were not detected in brain or plasma 90 minutes after their administration, neutral and negatively charged liposomes were able to reach the brain and accumulate specifically in the infarcted area. Moreover, neutral liposomes exhibited higher bioavailability in plasma 4 hours after being administered. The detection of simvastatin by ultra-high-protein liquid chromatography confirmed its ability to cross the blood–brain barrier, when administered either as a free drug or encapsulated into liposomes. Conclusion: This study confirms that liposome charge is critical to promote its accumulation in the brain infarct after MCAOt. Furthermore, simvastatin can be delivered after being encapsulated. Thus, simvastatin encapsulation might be a promising strategy to ensure that the drug reaches the brain, while increasing its bioavailability and reducing possible side effects. Keywords: simvastatin, liposomes, delivery, brain, stroke, rat

Published

2016

9. Vascular adhesion Protein-1 (VAP-1/sSAO) is involved in intracranial hemorrhagic complications after thrombolysis in human stroke

Author

Joan Montaner, Hernandez-Guillamon, M., Sole, M., Pares, M., Cuadrado, E., Valente, T., Garcia-Bonilla, L., Ribo, M., Rubiera, M., Molina, C., Alvarez-Sabin, J., Rosell, A., and Unzeta, M.

10. Brain perihematoma gene profile following spontaneous human intracerebral hemorrhage

Author

Rosell, A., Cuadrado, E., Ferandez-Cadenas, I., Delgado, P., Garcia, T., Ribo, M., Hernandez-Guillamon, M., Ortega-Aznar, A., and Joan Montaner

11. [The therapeutic potential of endothelial progenitor cells in ischaemic stroke]

Author

Navarro, M., Rosell, A., Hernandez-Guillamon, M., Cuadrado, E., and Joan Montaner

Subjects

Green Fluorescent Proteins, Hematopoietic Stem Cell Transplantation, Endothelial Cells, Neovascularization, Physiologic, Cell Differentiation, Flow Cytometry, Hematopoietic Stem Cells, Brain Ischemia, Rats, Mice, Cell Movement, Animals, Cytokines, Humans, Cell Lineage, Rabbits, Biomarkers, Cells, Cultured

Abstract

To review the present knowledge about endothelial progenitor cells (EPCs), their relationship with stroke and their possible therapeutic potential.Activation of angiogenesis and vasculogenesis after cerebral ischemia is an attempt to recover damaged cerebral tissue. The role of EPCs in angiogenesis/vasculogenesis after brain ischemia remains unknown. Many studies have been published about the isolation, phenotyping and function of EPCs. However, there is not a unique definition for these cells; their origin and function are still an issue of controversy between different research groups. In this review, we summarize the currently used techniques and the most relevant publications about EPCs in experimental models of cerebral ischemia and their role in stroke.The identification of EPCs in peripheral blood as hematopoietic cells with the ability to differentiate into endothelial cells, broke the paradigm that vasculogenesis was only an embryogenic process. However, better knowledge about the origin and function of EPCs in cerebral ischemia is required. Stimulation of these cells opens a wide new field of cell-based angiogenic therapy that could improve the current stroke treatment.

12. Dipyridamole confers protection in acute focal cerebral ischemia in the rat

Author

Garcia-Bonilla, L., Sosti, V., Hernandez-Guillamon, M., Rosell, A., and Joan Montaner

13. The Boston criteria version 2.0 for cerebral amyloid angiopathy: a multicentre, retrospective, MRI-neuropathology diagnostic accuracy study

Author

Andreas Charidimou, Gregoire Boulouis, Matthew P Frosch, Jean-Claude Baron, Marco Pasi, Jean Francois Albucher, Gargi Banerjee, Carmen Barbato, Fabrice Bonneville, Sebastian Brandner, Lionel Calviere, François Caparros, Barbara Casolla, Charlotte Cordonnier, Marie-Bernadette Delisle, Vincent Deramecourt, Martin Dichgans, Elif Gokcal, Jochen Herms, Mar Hernandez-Guillamon, Hans Rolf Jäger, Zane Jaunmuktane, Jennifer Linn, Sergi Martinez-Ramirez, Elena Martínez-Sáez, Christian Mawrin, Joan Montaner, Solene Moulin, Jean-Marc Olivot, Fabrizio Piazza, Laurent Puy, Nicolas Raposo, Mark A Rodrigues, Sigrun Roeber, Jose Rafael Romero, Neshika Samarasekera, Julie A Schneider, Stefanie Schreiber, Frank Schreiber, Corentin Schwall, Colin Smith, Levente Szalardy, Pascale Varlet, Alain Viguier, Joanna M Wardlaw, Andrew Warren, Frank A Wollenweber, Marialuisa Zedde, Mark A van Buchem, M Edip Gurol, Anand Viswanathan, Rustam Al-Shahi Salman, Eric E Smith, David J Werring, Steven M Greenberg, Charidimou, A, Boulouis, G, Frosch, M, Baron, J, Pasi, M, Albucher, J, Banerjee, G, Barbato, C, Bonneville, F, Brandner, S, Calviere, L, Caparros, F, Casolla, B, Cordonnier, C, Delisle, M, Deramecourt, V, Dichgans, M, Gokcal, E, Herms, J, Hernandez-Guillamon, M, Jäger, H, Jaunmuktane, Z, Linn, J, Martinez-Ramirez, S, Martínez-Sáez, E, Mawrin, C, Montaner, J, Moulin, S, Olivot, J, Piazza, F, Puy, L, Raposo, N, Rodrigues, M, Roeber, S, Romero, J, Samarasekera, N, Schneider, J, Schreiber, S, Schreiber, F, Schwall, C, Smith, C, Szalardy, L, Varlet, P, Viguier, A, Wardlaw, J, Warren, A, Wollenweber, F, Zedde, M, van Buchem, M, Gurol, M, Viswanathan, A, Al-Shahi Salman, R, Smith, E, Werring, D, and Greenberg, S

Subjects

diagnoisi, Amyloid beta-Peptides, pathology [Cerebral Hemorrhage], Middle Aged, MED/46 - SCIENZE TECNICHE DI MEDICINA DI LABORATORIO, Magnetic Resonance Imaging, diagnostic imaging [Cerebral Amyloid Angiopathy], Cerebral Amyloid Angiopathy, methods [Magnetic Resonance Imaging], biomarker, Humans, Neurology (clinical), ddc:610, Neuropathology, MRI, Aged, Cerebral Hemorrhage, Retrospective Studies

Abstract

BACKGROUND: Cerebral amyloid angiopathy (CAA) is an age-related small vessel disease, characterised pathologically by progressive deposition of amyloid β in the cerebrovascular wall. The Boston criteria are used worldwide for the in-vivo diagnosis of CAA but have not been updated since 2010, before the emergence of additional MRI markers. We report an international collaborative study aiming to update and externally validate the Boston diagnostic criteria across the full spectrum of clinical CAA presentations.METHODS: In this multicentre, hospital-based, retrospective, MRI and neuropathology diagnostic accuracy study, we did a retrospective analysis of clinical, radiological, and histopathological data available to sites participating in the International CAA Association to formulate updated Boston criteria and establish their diagnostic accuracy across different populations and clinical presentations. Ten North American and European academic medical centres identified patients aged 50 years and older with potential CAA-related clinical presentations (ie, spontaneous intracerebral haemorrhage, cognitive impairment, or transient focal neurological episodes), available brain MRI, and histopathological assessment for CAA diagnosis. MRI scans were centrally rated at Massachusetts General Hospital (Boston, MA, USA) for haemorrhagic and non-haemorrhagic CAA markers, and brain tissue samples were rated by neuropathologists at the contributing sites. We derived the Boston criteria version 2.0 (v2.0) by selecting MRI features to optimise diagnostic specificity and sensitivity in a prespecified derivation cohort (Boston cases 1994-2012, n=159), then externally validated the criteria in a prespecified temporal validation cohort (Boston cases 2012-18, n=59) and a geographical validation cohort (non-Boston cases 2004-18; n=123), comparing accuracy of the new criteria to the currently used modified Boston criteria with histopathological assessment of CAA as the diagnostic standard. We also assessed performance of the v2.0 criteria in patients across all cohorts who had the diagnostic gold standard of brain autopsy.FINDINGS: The study protocol was finalised on Jan 15, 2017, patient identification was completed on Dec 31, 2018, and imaging analyses were completed on Sept 30, 2019. Of 401 potentially eligible patients presenting to Massachusetts General Hospital, 218 were eligible to be included in the analysis; of 160 patient datasets from other centres, 123 were included. Using the derivation cohort, we derived provisional criteria for probable CAA requiring the presence of at least two strictly lobar haemorrhagic lesions (ie, intracerebral haemorrhages, cerebral microbleeds, or foci of cortical superficial siderosis) or at least one strictly lobar haemorrhagic lesion and at least one white matter characteristic (ie, severe visible perivascular spaces in centrum semiovale or white matter hyperintensities in a multispot pattern). The sensitivity and specificity of these criteria were 74·8% (95% CI 65·4-82·7) and 84·6% (71·9-93·1) in the derivation cohort, 92·5% (79·6-98·4) and 89·5% (66·9-98·7) in the temporal validation cohort, 80·2% (70·8-87·6) and 81·5% (61·9-93·7) in the geographical validation cohort, and 74·5% (65·4-82·4) and 95·0% (83·1-99·4) in all patients who had autopsy as the diagnostic standard. The area under the receiver operating characteristic curve (AUC) was 0·797 (0·732-0·861) in the derivation cohort, 0·910 (0·828-0·992) in the temporal validation cohort, 0·808 (0·724-0·893) in the geographical validation cohort, and 0·848 (0·794-0·901) in patients who had autopsy as the diagnostic standard. The v2.0 Boston criteria for probable CAA had superior accuracy to the current Boston criteria (sensitivity 64·5% [54·9-73·4]; specificity 95·0% [83·1-99·4]; AUC 0·798 [0·741-0854]; p=0·0005 for comparison of AUC) across all individuals who had autopsy as the diagnostic standard.INTERPRETATION: The Boston criteria v2.0 incorporate emerging MRI markers of CAA to enhance sensitivity without compromising their specificity in our cohorts of patients aged 50 years and older presenting with spontaneous intracerebral haemorrhage, cognitive impairment, or transient focal neurological episodes. Future studies will be needed to determine generalisability of the v.2.0 criteria across the full range of patients and clinical presentations.FUNDING: US National Institutes of Health (R01 AG26484).

Published

2021

14. Effects of Achieving Rapid, Intensive, and Sustained Blood Pressure Reduction in Intracerebral Hemorrhage Expansion and Functional Outcome.

Author

Rodriguez-Luna D, Pancorbo O, Llull L, Silva Y, Prats-Sanchez L, Muchada M, Rudilosso S, Terceño M, Ramos-Pachón A, Hernandez Guillamon M, Coscojuela P, Blasco J, Perez-Hoyos S, Chamorro A, and Molina CA

Subjects

Adult, Humans, Male, Middle Aged, Aged, Aged, 80 and over, Female, Blood Pressure physiology, Antihypertensive Agents therapeutic use, Antihypertensive Agents pharmacology, Prospective Studies, Cerebral Hemorrhage diagnostic imaging, Cerebral Hemorrhage drug therapy, Hematoma diagnostic imaging, Hematoma drug therapy, Treatment Outcome, Stroke drug therapy, Hypotension

Abstract

Background and Objectives: The time taken to achieve blood pressure (BP) control could be pivotal in the benefits of reducing BP in acute intracerebral hemorrhage (ICH). We aimed to assess the relationship between the rapid achievement and sustained maintenance of an intensive systolic BP (SBP) target with radiologic, clinical, and functional outcomes., Methods: Rapid, Intensive, and Sustained BP lowering in Acute ICH (RAINS) was a multicenter, prospective, observational cohort study of adult patients with ICH <6 hours and SBP ≥150 mm Hg at 4 Comprehensive Stroke Centers during a 4.5-year period. Patients underwent baseline and 24-hour CT scans and 24-hour noninvasive BP monitoring. BP was managed under a rapid (target achievement ≤60 minutes), intensive (target SBP <140 mm Hg), and sustained (target stability for 24 hours) BP protocol. SBP target achievement ≤60 minutes and 24-hour SBP variability were recorded. Outcomes included hematoma expansion (>6 mL or >33%) at 24 hours (primary outcome), early neurologic deterioration (END, 24-hour increase in NIH Stroke Scale score ≥4), and 90-day ordinal modified Rankin scale (mRS) score. Analyses were adjusted by age, sex, anticoagulation, onset-to-imaging time, ICH volume, and intraventricular extension., Results: We included 312 patients (mean age 70.2 ± 13.3 years, 202 [64.7%] male). Hematoma expansion occurred in 70/274 (25.6%) patients, END in 58/291 (19.9%), and the median 90-day mRS score was 4 (interquartile range, 2-5). SBP target achievement ≤60 minutes (178/312 [57.1%]) associated with a lower risk of hematoma expansion (adjusted odds ratio [aOR] 0.43, 95% confidence interval [CI] 0.23-0.77), lower END rate (aOR 0.43, 95% CI 0.23-0.80), and lower 90-day mRS scores (aOR 0.48, 95% CI 0.32-0.74). The mean 24-hour SBP variability was 21.0 ± 7.6 mm Hg. Higher 24-hour SBP variability was not related to expansion (aOR 0.99, 95% CI 0.95-1.04) but associated with higher END rate (aOR 1.15, 95% CI 1.09-1.21) and 90-day mRS scores (aOR 1.06, 95% CI 1.04-1.10)., Discussion: Among patients with acute ICH, achieving an intensive SBP target within 60 minutes was associated with lower hematoma expansion risk. Rapid SBP reduction and stable sustention within 24 hours were related to improved clinical and functional outcomes. These findings warrant the design of randomized clinical trials examining the impact of effectively achieving rapid, intensive, and sustained BP control on hematoma expansion., Classification of Evidence: This study provides Class III evidence that in adults with spontaneous ICH and initial SBP ≥150 mm Hg, lowering SBP to <140 mm Hg within the first hour and maintaining this for 24 hours is associated with decreased hematoma expansion.

Published

2024

15. Implications of a pathophysiological framework for cerebral amyloid angiopathy.

Author

Hernandez-Guillamon M

Subjects

Humans, Cerebral Hemorrhage, Amyloid beta-Peptides, Cerebral Amyloid Angiopathy complications

Abstract

Competing Interests: I declare no competing interests.

Published

2023

16. The Boston criteria version 2.0 for cerebral amyloid angiopathy: a multicentre, retrospective, MRI-neuropathology diagnostic accuracy study.

Author

Charidimou A, Boulouis G, Frosch MP, Baron JC, Pasi M, Albucher JF, Banerjee G, Barbato C, Bonneville F, Brandner S, Calviere L, Caparros F, Casolla B, Cordonnier C, Delisle MB, Deramecourt V, Dichgans M, Gokcal E, Herms J, Hernandez-Guillamon M, Jäger HR, Jaunmuktane Z, Linn J, Martinez-Ramirez S, Martínez-Sáez E, Mawrin C, Montaner J, Moulin S, Olivot JM, Piazza F, Puy L, Raposo N, Rodrigues MA, Roeber S, Romero JR, Samarasekera N, Schneider JA, Schreiber S, Schreiber F, Schwall C, Smith C, Szalardy L, Varlet P, Viguier A, Wardlaw JM, Warren A, Wollenweber FA, Zedde M, van Buchem MA, Gurol ME, Viswanathan A, Al-Shahi Salman R, Smith EE, Werring DJ, and Greenberg SM

Subjects

Aged, Amyloid beta-Peptides, Cerebral Hemorrhage pathology, Humans, Magnetic Resonance Imaging methods, Middle Aged, Retrospective Studies, Cerebral Amyloid Angiopathy diagnostic imaging, Neuropathology

Abstract

Background: Cerebral amyloid angiopathy (CAA) is an age-related small vessel disease, characterised pathologically by progressive deposition of amyloid β in the cerebrovascular wall. The Boston criteria are used worldwide for the in-vivo diagnosis of CAA but have not been updated since 2010, before the emergence of additional MRI markers. We report an international collaborative study aiming to update and externally validate the Boston diagnostic criteria across the full spectrum of clinical CAA presentations., Methods: In this multicentre, hospital-based, retrospective, MRI and neuropathology diagnostic accuracy study, we did a retrospective analysis of clinical, radiological, and histopathological data available to sites participating in the International CAA Association to formulate updated Boston criteria and establish their diagnostic accuracy across different populations and clinical presentations. Ten North American and European academic medical centres identified patients aged 50 years and older with potential CAA-related clinical presentations (ie, spontaneous intracerebral haemorrhage, cognitive impairment, or transient focal neurological episodes), available brain MRI, and histopathological assessment for CAA diagnosis. MRI scans were centrally rated at Massachusetts General Hospital (Boston, MA, USA) for haemorrhagic and non-haemorrhagic CAA markers, and brain tissue samples were rated by neuropathologists at the contributing sites. We derived the Boston criteria version 2.0 (v2.0) by selecting MRI features to optimise diagnostic specificity and sensitivity in a prespecified derivation cohort (Boston cases 1994-2012, n=159), then externally validated the criteria in a prespecified temporal validation cohort (Boston cases 2012-18, n=59) and a geographical validation cohort (non-Boston cases 2004-18; n=123), comparing accuracy of the new criteria to the currently used modified Boston criteria with histopathological assessment of CAA as the diagnostic standard. We also assessed performance of the v2.0 criteria in patients across all cohorts who had the diagnostic gold standard of brain autopsy., Findings: The study protocol was finalised on Jan 15, 2017, patient identification was completed on Dec 31, 2018, and imaging analyses were completed on Sept 30, 2019. Of 401 potentially eligible patients presenting to Massachusetts General Hospital, 218 were eligible to be included in the analysis; of 160 patient datasets from other centres, 123 were included. Using the derivation cohort, we derived provisional criteria for probable CAA requiring the presence of at least two strictly lobar haemorrhagic lesions (ie, intracerebral haemorrhages, cerebral microbleeds, or foci of cortical superficial siderosis) or at least one strictly lobar haemorrhagic lesion and at least one white matter characteristic (ie, severe visible perivascular spaces in centrum semiovale or white matter hyperintensities in a multispot pattern). The sensitivity and specificity of these criteria were 74·8% (95% CI 65·4-82·7) and 84·6% (71·9-93·1) in the derivation cohort, 92·5% (79·6-98·4) and 89·5% (66·9-98·7) in the temporal validation cohort, 80·2% (70·8-87·6) and 81·5% (61·9-93·7) in the geographical validation cohort, and 74·5% (65·4-82·4) and 95·0% (83·1-99·4) in all patients who had autopsy as the diagnostic standard. The area under the receiver operating characteristic curve (AUC) was 0·797 (0·732-0·861) in the derivation cohort, 0·910 (0·828-0·992) in the temporal validation cohort, 0·808 (0·724-0·893) in the geographical validation cohort, and 0·848 (0·794-0·901) in patients who had autopsy as the diagnostic standard. The v2.0 Boston criteria for probable CAA had superior accuracy to the current Boston criteria (sensitivity 64·5% [54·9-73·4]; specificity 95·0% [83·1-99·4]; AUC 0·798 [0·741-0854]; p=0·0005 for comparison of AUC) across all individuals who had autopsy as the diagnostic standard., Interpretation: The Boston criteria v2.0 incorporate emerging MRI markers of CAA to enhance sensitivity without compromising their specificity in our cohorts of patients aged 50 years and older presenting with spontaneous intracerebral haemorrhage, cognitive impairment, or transient focal neurological episodes. Future studies will be needed to determine generalisability of the v.2.0 criteria across the full range of patients and clinical presentations., Funding: US National Institutes of Health (R01 AG26484)., Competing Interests: Declaration of interests AC reports receiving funding from the Bodossaki Foundation and the Frechette Family Foundation and consulting fees from Imperative Care. MPF reports receiving funding from Biogen and Voyager Therapeutics. Gba reports receiving funding from the Rosetrees Trust, Alzheimer's Research UK, NIHR, and the Stroke Association. CC reports receiving funding from the French Ministry of Health and honoraria from Amgen, and participating in data safety monitoring, advisory, or steering committees for the University of Glasgow, University of Caen, Op2Lysis, AstraZeneca, Bristol Myers Squibb, and Biogen. MD reports receiving funding from Deutsche Forschungsgemeinschaft under Germany's Excellence Strategy within the framework of the Munich Cluster for Systems Neurology and the Vascular Dementia Research Foundation. JH reports receiving funding from the German Research Foundation and German Center for Neurodegenerative Diseases and tissue from Neurobiobank Munich. JL reports serving on a serving on an advisory board for Biogen and Mediaire. LP reports receiving honoraria from Daiichi Sankyo Ireland. FP reports receiving funding from the Alzheimer's Association (AARG-18-561699), participation on an Advisory Board for Roche, and leadership of the CAA Study Group of the Italia Society of Neurology-Dementia and the iCAB International Network. SR reports receiving funding from the German Research Foundation and brain tissue from Neurobiobank Munich. MAR reports receiving funding from the Wellcome Trust. JAS reports receiving funding from the US National Institutes of Health, consulting fees from Alnylam Pharmaceuticals, Apellis Pharmaceuticals, and Avid Radiopharmaceuticals, honoraria from Weil Cornell University, payment for expert testimony from the National Hockey League, support for travel from the US National Institutes for Health, serving on safety monitoring or advisory boards for the Framingham Heart Study, DISCOVERY, University of Kansas, Boston University, and University of California Irvine, and serving in leadership positions for the Alzheimer's Association and Foundation Alzheimer France. CSm reports receiving funding from the Medical Research Council UK. LS reports receiving funding from the Hungarian Academy of Sciences and Ministry for Innovation and Technology of Hungary from the source of the National Research. JMW reports receiving funding from the UK Dementia Research Institute funded by the UK Medical Research Council, Alzheimer's Society, and Alzheimer's Research UK, and a leadership role for the European Stroke Organization SVD Guidelines. FAW reports receiving honoraria from Alexion Pharm. MEG reports receiving funding from Avid Radiopharmaceuticals, Pfizer, and Boston Scientific. AV reports receiving funding from the US National Institutes of Health and consulting fees from Alnylam Pharmaceuticals and Biogen Pharmaceuticals. RA-SS reports receiving funding from the UK Medical Research Council and the Stroke Association. EES reports receiving funding from the Canadian Institutes of Health Research, Brain Canada, and Biogen, and consulting fees from Biogen and Eli Lily. DJW reports receiving consulting fees from Alnylam and Novo Nordisk, honoraria from Bayer and Alexion, participation on a safety monitoring board for the OXHARP study, and serving in leadership for the British Association of Stroke Physicians. SMG reports receiving funding from the US National Institutes of Health, royalties from Up-To-Date, consulting fees from Eli Lily, and serving on data safety monitoring committees for Washington University, Bayer, Biogen, and Roche. All other authors declare no competing interests., (Copyright © 2022 Elsevier Ltd. All rights reserved.)

Published

2022

17. Cerebral amyloid angiopathy and Alzheimer disease - one peptide, two pathways.

Author

Greenberg SM, Bacskai BJ, Hernandez-Guillamon M, Pruzin J, Sperling R, and van Veluw SJ

Subjects

Alzheimer Disease genetics, Alzheimer Disease pathology, Amyloid beta-Peptides genetics, Brain pathology, Cerebral Amyloid Angiopathy genetics, Cerebral Amyloid Angiopathy pathology, Humans, Plaque, Amyloid genetics, Plaque, Amyloid metabolism, Plaque, Amyloid pathology, Alzheimer Disease metabolism, Amyloid beta-Peptides metabolism, Brain metabolism, Cerebral Amyloid Angiopathy metabolism, Signal Transduction physiology

Abstract

The shared role of amyloid-β (Aβ) deposition in cerebral amyloid angiopathy (CAA) and Alzheimer disease (AD) is arguably the clearest instance of crosstalk between neurodegenerative and cerebrovascular processes. The pathogenic pathways of CAA and AD intersect at the levels of Aβ generation, its circulation within the interstitial fluid and perivascular drainage pathways and its brain clearance, but diverge in their mechanisms of brain injury and disease presentation. Here, we review the evidence for and the pathogenic implications of interactions between CAA and AD. Both pathologies seem to be driven by impaired Aβ clearance, creating conditions for a self-reinforcing cycle of increased vascular Aβ, reduced perivascular clearance and further CAA and AD progression. Despite the close relationship between vascular and plaque Aβ deposition, several factors favour one or the other, such as the carboxy-terminal site of the peptide and specific co-deposited proteins. Amyloid-related imaging abnormalities that have been seen in trials of anti-Aβ immunotherapy are another probable intersection between CAA and AD, representing overload of perivascular clearance pathways and the effects of removing Aβ from CAA-positive vessels. The intersections between CAA and AD point to a crucial role for improving vascular function in the treatment of both diseases and indicate the next steps necessary for identifying therapies.

Published

2020

18. Advancing diagnostic criteria for sporadic cerebral amyloid angiopathy: Study protocol for a multicenter MRI-pathology validation of Boston criteria v2.0.

Author

Charidimou A, Frosch MP, Al-Shahi Salman R, Baron JC, Cordonnier C, Hernandez-Guillamon M, Linn J, Raposo N, Rodrigues M, Romero JR, Schneider JA, Schreiber S, Smith EE, van Buchem MA, Viswanathan A, Wollenweber FA, Werring DJ, and Greenberg SM

Subjects

Cerebral Amyloid Angiopathy diagnosis, Cerebral Amyloid Angiopathy pathology, Humans, Magnetic Resonance Imaging, Reproducibility of Results, Sensitivity and Specificity, Cerebral Amyloid Angiopathy diagnostic imaging

Abstract

Rationale: The Boston criteria are used worldwide for the in vivo diagnosis of cerebral amyloid angiopathy and are the basis for clinical decision-making and research in the field. Given substantial advances in cerebral amyloid angiopathy's clinical aspects and MRI biomarkers, we designed a multicenter study within the International cerebral amyloid angiopathy Association aimed at further validating the diagnostic accuracy of the Boston and potentially improving and updating them., Aim: We aim to derive and validate an updated "version 2.0" of the Boston criteria across the spectrum of cerebral amyloid angiopathy-related presentations and MRI biomarkers., Sample Size Estimates: Participating centers with suitable available data (see Methods) were identified from existing collaborations and an open invitation to the International Cerebral Amyloid Angiopathy Association emailing list. Our study sample will include: (1) a derivation cohort - Massachusetts General Hospital (MGH), Boston cases from inception to 2012 (∼150 patients); (2) temporal external validation cohort - MGH, Boston cases from 2012 to 2018 (∼100 patients); and (3) geographical external validation cohort - non-Boston cases (∼85 patients)., Methods and Design: Multicenter collaborative study. We will collect and analyze data from patients' age ≥ 50 with any potential sporadic cerebral amyloid angiopathy-related clinical presentations (spontaneous intracerebral hemorrhage, transient focal neurological episodes and cognitive impairment), available brain MRI ("index test"), and histopathologic assessment for cerebral amyloid angiopathy ("reference standard" for diagnosis). Trained raters will assess MRI for all prespecified hemorrhagic and non-hemorrhagic small vessel disease markers of interest, according to validated criteria and a prespecified protocol, masked to clinical and histopathologic features. Brain tissue samples will be rated for cerebral amyloid angiopathy, defined as Vonsattel grade ≥2 for whole brain autopsies and ≥1 for cortical biopsies or hematoma evacuation. Based on our estimated available sample size, we will undertake pre-specified cohort splitting as above. We will: (a) pre-specify variables and statistical cut-offs; (b) examine univariable and multivariable associations; and (c) then assess classification measures (sensitivity, specificity etc.) for each MRI biomarker individually, in relation to the cerebral amyloid angiopathy diagnosis reference standard on neuropathology in a derivation cohort. The MRI biomarkers strongly associated with cerebral amyloid angiopathy diagnosis will be selected for inclusion in provisional (probable and possible cerebral amyloid angiopathy) Boston criteria v2.0 and validated using appropriate metrics and models., Study Outcomes: Boston criteria v2.0 for clinical cerebral amyloid angiopathy diagnosis., Discussion: This work aims to potentially update and improve the diagnostic test accuracy of the Boston criteria for cerebral amyloid angiopathy and to provide wider validation of the criteria in a large sample. We envision that this work will meet the needs of clinicians and investigators and help accelerate progress towards better treatment of cerebral amyloid angiopathy.

Published

2019

19. PATJ Low Frequency Variants Are Associated With Worse Ischemic Stroke Functional Outcome.

Author

Mola-Caminal M, Carrera C, Soriano-Tárraga C, Giralt-Steinhauer E, Díaz-Navarro RM, Tur S, Jiménez C, Medina-Dols A, Cullell N, Torres-Aguila NP, Muiño E, Rodríguez-Campello A, Ois A, Cuadrado-Godia E, Vivanco-Hidalgo RM, Hernandez-Guillamon M, Solé M, Delgado P, Bustamante A, García-Berrocoso T, Mendióroz M, Castellanos M, Serena J, Martí-Fàbregas J, Segura T, Serrano-Heras G, Obach V, Ribó M, Molina CA, Alvarez-Sabín J, Palomeras E, Freijo M, Font MA, Rosand J, Rost NS, Gallego-Fabrega C, Lee JM, Heitsch L, Ibanez L, Cruchaga C, Phuah CL, Lemmens R, Thijs V, Lindgren A, Maguire J, Rannikmae K, Sudlow CL, Jern C, Stanne TM, Lorentzen E, Muñoz-Narbona L, Dávalos A, López-Cancio E, Worrall BB, Woo D, Kittner SJ, Mitchell BD, Montaner J, Roquer J, Krupinski J, Estivill X, Rabionet R, Vives-Bauzá C, Fernández-Cadenas I, and Jiménez-Conde J

Subjects

Brain Ischemia diagnosis, Brain Ischemia physiopathology, Brain Ischemia rehabilitation, Disability Evaluation, Gene Frequency, Genetic Predisposition to Disease, Genome-Wide Association Study, Humans, Phenotype, Recovery of Function, Risk Factors, Stroke diagnosis, Stroke physiopathology, Stroke therapy, Stroke Rehabilitation, Treatment Outcome, Brain Ischemia genetics, Polymorphism, Single Nucleotide, Stroke genetics, Tight Junction Proteins genetics

Abstract

Rationale: Ischemic stroke is among the leading causes of adult disability. Part of the variability in functional outcome after stroke has been attributed to genetic factors but no locus has been consistently associated with stroke outcome., Objective: Our aim was to identify genetic loci influencing the recovery process using accurate phenotyping to produce the largest GWAS (genome-wide association study) in ischemic stroke recovery to date., Methods and Results: A 12-cohort, 2-phase (discovery-replication and joint) meta-analysis of GWAS included anterior-territory and previously independent ischemic stroke cases. Functional outcome was recorded using 3-month modified Rankin Scale. Analyses were adjusted for confounders such as discharge National Institutes of Health Stroke Scale. A gene-based burden test was performed. The discovery phase (n=1225) was followed by open (n=2482) and stringent joint-analyses (n=1791). Those cohorts with modified Rankin Scale recorded at time points other than 3-month or incomplete data on previous functional status were excluded in the stringent analyses. Novel variants in PATJ (Pals1-associated tight junction) gene were associated with worse functional outcome at 3-month after stroke. The top variant was rs76221407 (G allele, β=0.40, P=1.70×10 -9 )., Conclusions: Our results identify a set of common variants in PATJ gene associated with 3-month functional outcome at genome-wide significance level. Future studies should examine the role of PATJ in stroke recovery and consider stringent phenotyping to enrich the information captured to unveil additional stroke outcome loci.

Published

2019

20. Brain hemorrhage recurrence, small vessel disease type, and cerebral microbleeds: A meta-analysis.

Author

Charidimou A, Imaizumi T, Moulin S, Biffi A, Samarasekera N, Yakushiji Y, Peeters A, Vandermeeren Y, Laloux P, Baron JC, Hernandez-Guillamon M, Montaner J, Casolla B, Gregoire SM, Kang DW, Kim JS, Naka H, Smith EE, Viswanathan A, Jäger HR, Al-Shahi Salman R, Greenberg SM, Cordonnier C, and Werring DJ

Subjects

Brain diagnostic imaging, Humans, Magnetic Resonance Imaging, Recurrence, Risk, Cerebral Hemorrhage diagnostic imaging, Cerebral Hemorrhage epidemiology

Abstract

Objective: We evaluated recurrent intracerebral hemorrhage (ICH) risk in ICH survivors, stratified by the presence, distribution, and number of cerebral microbleeds (CMBs) on MRI (i.e., the presumed causal underlying small vessel disease and its severity)., Methods: This was a meta-analysis of prospective cohorts following ICH, with blood-sensitive brain MRI soon after ICH. We estimated annualized recurrent symptomatic ICH rates for each study and compared pooled odds ratios (ORs) of recurrent ICH by CMB presence/absence and presumed etiology based on CMB distribution (strictly lobar CMBs related to probable or possible cerebral amyloid angiopathy [CAA] vs non-CAA) and burden (1, 2-4, 5-10, and >10 CMBs), using random effects models., Results: We pooled data from 10 studies including 1,306 patients: 325 with CAA-related and 981 CAA-unrelated ICH. The annual recurrent ICH risk was higher in CAA-related ICH vs CAA-unrelated ICH (7.4%, 95% confidence interval [CI] 3.2-12.6 vs 1.1%, 95% CI 0.5-1.7 per year, respectively; p = 0.01). In CAA-related ICH, multiple baseline CMBs (versus none) were associated with ICH recurrence during follow-up (range 1-3 years): OR 3.1 (95% CI 1.4-6.8; p = 0.006), 4.3 (95% CI 1.8-10.3; p = 0.001), and 3.4 (95% CI 1.4-8.3; p = 0.007) for 2-4, 5-10, and >10 CMBs, respectively. In CAA-unrelated ICH, only >10 CMBs (versus none) were associated with recurrent ICH (OR 5.6, 95% CI 2.1-15; p = 0.001). The presence of 1 CMB (versus none) was not associated with recurrent ICH in CAA-related or CAA-unrelated cohorts., Conclusions: CMB burden and distribution on MRI identify subgroups of ICH survivors with higher ICH recurrence risk, which may help to predict ICH prognosis with relevance for clinical practice and treatment trials., (Copyright © 2017 The Author(s). Published by Wolters Kluwer Health, Inc. on behalf of the American Academy of Neurology.)

Published

2017

21. Sequential Amyloid-β Degradation by the Matrix Metalloproteases MMP-2 and MMP-9.

Author

Hernandez-Guillamon M, Mawhirt S, Blais S, Montaner J, Neubert TA, Rostagno A, and Ghiso J

Subjects

Blotting, Western, Cell Line, Tumor, Enzyme-Linked Immunosorbent Assay, Humans, Proteolysis, Recombinant Proteins metabolism, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Amyloid beta-Peptides metabolism, Matrix Metalloproteinase 2 metabolism, Matrix Metalloproteinase 9 metabolism

Abstract

Matrix metalloproteases (MMPs) MMP-2 and MMP-9 have been implicated in the physiological catabolism of Alzheimer's amyloid-β (Aβ). Conversely, their association with vascular amyloid deposits, blood-brain barrier disruption, and hemorrhagic transformations after ischemic stroke also highlights their involvement in pathological processes. To better understand this dichotomy, recombinant human (rh) MMP-2 and MMP-9 were incubated with Aβ40 and Aβ42, and the resulting proteolytic fragments were assessed via immunoprecipitation and quantitative mass spectrometry. Both MMPs generated Aβ fragments truncated only at the C terminus, ending at positions 34, 30, and 16. Using deuterated homologues as internal standards, we observed limited and relatively slow degradation of Aβ42 by rhMMP-2, although the enzyme cleaved >80% of Aβ40 during the 1st h of incubation. rhMMP-9 was significantly less effective, particularly in degrading Aβ(1-42), although the targeted peptide bonds were identical. Using Aβ(1-34) and Aβ(1-30), we demonstrated that these peptides are also substrates for both MMPs, cleaving Aβ(1-34) to produce Aβ(1-30) first and Aβ(1-16) subsequently. Consistent with the kinetics observed with full-length Aβ, rhMMP-9 degraded only a minute fraction of Aβ(1-34) and was even less effective in producing Aβ(1-16). Further degradation of Aβ(1-16) by either MMP-2 or MMP-9 was not observed even after prolonged incubation times. Notably, all MMP-generated C-terminally truncated Aβ fragments were highly soluble and did not exhibit fibrillogenic properties or induce cytotoxicity in human cerebral microvascular endothelial or neuronal cells supporting the notion that these truncated Aβ species are associated with clearance mechanisms rather than being key elements in the fibrillogenesis process., (© 2015 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2015

22. Matrix Metalloproteinases in Alzheimer's Disease and Concurrent Cerebral Microbleeds.

Author

Duits FH, Hernandez-Guillamon M, Montaner J, Goos JD, Montañola A, Wattjes MP, Barkhof F, Scheltens P, Teunissen CE, and van der Flier WM

Subjects

Aged, Alzheimer Disease pathology, Amyloid beta-Peptides cerebrospinal fluid, Biomarkers cerebrospinal fluid, Blood Chemical Analysis, Brain pathology, Cerebral Hemorrhage pathology, Enzyme-Linked Immunosorbent Assay, Female, Humans, Magnetic Resonance Imaging, Male, Peptide Fragments cerebrospinal fluid, Phosphorylation, Tissue Inhibitor of Metalloproteinases blood, Tissue Inhibitor of Metalloproteinases cerebrospinal fluid, tau Proteins cerebrospinal fluid, Alzheimer Disease physiopathology, Brain physiopathology, Cerebral Hemorrhage physiopathology, Matrix Metalloproteinases blood, Matrix Metalloproteinases cerebrospinal fluid

Abstract

Matrix metalloproteinases (MMPs) are a family of enzymes able to degrade components of the extracellular matrix, which is important for normal blood-brain barrier function. Their function is regulated by tissue inhibitors of matrix metalloproteinases (TIMPs). We investigated whether MMPs and TIMPs in cerebrospinal fluid (CSF) and plasma were altered in Alzheimer's disease (AD) and vascular dementia (VaD), and whether this effect was modified by presence of cerebral micro-bleeds in AD patients. In addition, we assessed associations of MMPs and TIMPs with CSF amyloid-β(1-42) (Aβ42), tau, and tau phosphorylated at threonine-181 (p-tau). We measured MMP2, MMP9, and MMP10, and TIMP1 and TIMP2 in CSF and plasma of 52 AD patients, 26 matched controls, and 24 VaD patients. AD patients showed higher plasma MMP2 levels compared to VaD patients (p <  0.05), and higher CSF MMP10 levels compared to controls (p <  0.05). Microbleeds in AD were associated with lower CSF TIMP1, TIMP2 and MMP9 in a dose-response relation. In addition, CSF MMP2 was associated with p-tau (St.B 0.23, p <  0.05), and CSF MMP10 with tau (St.B 0.38, p <  0.001) and p-tau (St.B 0.40, p <  0.001). Our findings suggest involvement of MMP2 and MMP10 in AD pathology. Lower levels of TIMPs in AD patients with microbleeds suggest less MMP inhibition in patients with concurrent cerebral microbleeds, which may hypothetically lead to a more vulnerable blood-brain barrier in these patients.

Published

2015

23. Genes involved in hemorrhagic transformations that follow recombinant t-PA treatment in stroke patients.

Author

Fernandez-Cadenas I, Del Rio-Espinola A, Domingues-Montanari S, Mendioroz M, Fernandez-Morales J, Penalba A, Rubiera M, Hernandez-Guillamon M, Rosell A, Delgado P, Chacon P, Ribo M, Alvarez-Sabin J, Molina CA, García-Arumi E, and Montaner J

Subjects

Apoptosis genetics, Drug-Related Side Effects and Adverse Reactions pathology, Female, Gene Regulatory Networks, Hemorrhage complications, Hemorrhage pathology, Humans, Male, Neutrophils metabolism, Recombinant Proteins administration & dosage, Recombinant Proteins adverse effects, Stroke complications, Stroke drug therapy, Stroke pathology, Tissue Plasminogen Activator administration & dosage, Tissue Plasminogen Activator adverse effects, Treatment Outcome, Drug-Related Side Effects and Adverse Reactions genetics, Hemorrhage chemically induced, Hemorrhage genetics, Stroke genetics

Abstract

Aim: Despite the benefits of recombinant t-PA (rt-PA) for stroke patients some of them suffer from adverse hemorrhagic transformations (HTs) following treatment. Our objective is to study the transcriptomics of HTs patients., Methods: We studied by microarrays 11 blood samples from patients with stroke that had received rt-PA of whom six of them had suffered a HT. For replication step RNA was collected from 14 new subjects (seven with HT, seven without) and then analyzed by real-time PCR. Four proteins were measured by ELISA in 72 new subjects to analyze their role as potential protein biomarkers., Results: The microarray analysis revealed that 14 genes were altered among the HT patients. The replication study confirmed these results for six genes. Two of them (BCL2 and OLFM4) are associated with apoptosis, whereas the other four (LTF, LCN2 [also known as NGAL], CEACAM8 and CRISP3) are involved in the regulation of neutrophil processes., Conclusion: Our data revealed that genes related to apoptosis and neutrophil regulation pathways could be associated with HTs after rt-PA.

Published

2013

24. MMP-2/MMP-9 plasma level and brain expression in cerebral amyloid angiopathy-associated hemorrhagic stroke.

Author

Hernandez-Guillamon M, Martinez-Saez E, Delgado P, Domingues-Montanari S, Boada C, Penalba A, Boada M, Pagola J, Maisterra O, Rodriguez-Luna D, Molina CA, Rovira A, Alvarez-Sabin J, Ortega-Aznar A, and Montaner J

Subjects

Aged, Aged, 80 and over, Amyloid beta-Peptides blood, Brain blood supply, Brain pathology, Cerebral Amyloid Angiopathy blood, Cerebral Amyloid Angiopathy pathology, Cerebral Hemorrhage blood, Cerebral Hemorrhage pathology, Female, Humans, Inflammation blood, Inflammation enzymology, Inflammation pathology, Male, Middle Aged, Stroke blood, Stroke pathology, Brain enzymology, Cerebral Amyloid Angiopathy enzymology, Cerebral Hemorrhage enzymology, Matrix Metalloproteinase 2 blood, Matrix Metalloproteinase 9 blood, Stroke enzymology

Abstract

Cerebral amyloid angiopathy (CAA) is one of the main causes of intracerebral hemorrhage (ICH) in the elderly. Matrix metalloproteinases (MMPs) have been implicated in blood-brain barrier disruption and ICH pathogenesis. In this study, we determined the levels MMP-2 and MMP-9 in plasma and their brain expression in CAA-associated hemorrhagic stroke. Although MMP-2 and MMP-9 plasma levels did not differ among patients and controls, their brain expression was increased in perihematoma areas of CAA-related hemorrhagic strokes compared with contralateral areas and nonhemorrhagic brains. In addition, MMP-2 reactivity was found in β-amyloid (Aβ)-damaged vessels located far from the acute ICH and in chronic microbleeds. MMP-2 expression was associated to endothelial cells, histiocytes and reactive astrocytes, whereas MMP-9 expression was restricted to inflammatory cells. In summary, MMP-2 expression within and around Aβ-compromised vessels might contribute to the vasculature fatal fate, triggering an eventual bleeding., (© 2011 The Authors. Brain Pathology © 2011 International Society of Neuropathology.)

Published

2012

25. VAP-1/SSAO plasma activity and brain expression in human hemorrhagic stroke.

Author

Hernandez-Guillamon M, Solé M, Delgado P, García-Bonilla L, Giralt D, Boada C, Penalba A, García S, Flores A, Ribó M, Alvarez-Sabin J, Ortega-Aznar A, Unzeta M, and Montaner J

Subjects

Aged, Aged, 80 and over, Autopsy, Biomarkers blood, Blotting, Western, Case-Control Studies, Chi-Square Distribution, Female, Humans, Immunohistochemistry, Intracranial Hemorrhages blood, Intracranial Hemorrhages mortality, Logistic Models, Male, Middle Aged, Multivariate Analysis, Odds Ratio, Prognosis, Spain, Stroke blood, Stroke mortality, Time Factors, Up-Regulation, Amine Oxidase (Copper-Containing) blood, Brain enzymology, Cell Adhesion Molecules blood, Intracranial Hemorrhages enzymology, Stroke enzymology

Abstract

Background: Vascular adhesion protein-1 (VAP-1) is a cell surface and circulating enzyme that belongs to the semicarbazide-sensitive amine oxidase (SSAO) family, which oxidatively deaminates primary amines and is implicated in leukocyte extravasation. Our aim was to investigate the alteration of soluble VAP-1/SSAO activity in plasma samples after acute intracerebral hemorrhage (ICH) and its presence in human ICH brain tissue., Methods: VAP-1/SSAO activity was determined in plasma of 66 ICH patients and 58 healthy controls. In addition, we assessed the expression of VAP-1/SSAO in postmortem brain tissue from hemorrhagic stroke patients by Western blot and immunohistochemistry., Results: We observed significantly higher levels of plasma VAP-1/SSAO activity in patients with ICH compared to matched elderly controls (p = 0.001). Plasma VAP-1/SSAO activity <2.7 pmol/min·mg and baseline ICH volume <17 ml were independent predictors of neurological improvement after 48 h (OR 6.8, 95% CI 1.14-41.67, p = 0.035, and OR 10.64, 95% CI 1.1-100, p = 0.041, respectively), after adjustment for baseline stroke severity. We also found that membrane-bound VAP-1/SSAO levels were lower in the perihematoma region than in the corresponding contralateral brain areas of patients deceased due to ICH (p = 0.024)., Conclusions: Our data demonstrate that plasma VAP-1/SSAO activity is increased in ICH and predicts neurological outcome, suggesting a possible contribution of the soluble protein in secondary brain damage. Furthermore, anti-VAP-1/SSAO strategies might be a promising approach to prevent neurological worsening following ICH., (Copyright © 2011 S. Karger AG, Basel.)

Published

2012

26. Plasma β-amyloid levels in cerebral amyloid angiopathy-associated hemorrhagic stroke.

Author

Hernandez-Guillamon M, Delgado P, Penalba A, Rodriguez-Luna D, Molina CA, Rovira A, Alvarez-Sabin J, Boada M, and Montaner J

Subjects

Aged, Aged, 80 and over, Amyloid beta-Peptides classification, Analysis of Variance, Female, Humans, Male, Middle Aged, Peptide Fragments blood, Amyloid beta-Peptides blood, Cerebral Amyloid Angiopathy blood, Cerebral Amyloid Angiopathy complications, Cerebral Hemorrhage blood, Cerebral Hemorrhage etiology

Abstract

Background: Cerebral amyloid angiopathy (CAA) is one of the main causes of intracerebral hemorrhage (ICH) in the elderly., Objective: To analyze β-amyloid (Aβ) species in plasma in order to uncover biological markers that may contribute to improve the diagnosis of CAA in life., Methods: We determined the level of Aβ(1-40), Aβ(N-40), Aβ(1-42) and Aβ(N-42) in plasma of CAA-related ICH patients (n = 29) and healthy controls (n = 21) using xMAP® technology. Hemorrhages were identified and classified using a CT scan and brain MRI. Patients were clinically classified as probable or possible CAA according to the Boston criteria., Results: We found that plasma full-length Aβ(1-42) and truncated fragments Aβ(N-42) were higher in probable CAA patients than in controls (p < 0.001 and p = 0.046, respectively), and full-length Aβ(1-40) was selectively elevated in probable CAA compared to possible cases (p = 0.015) and controls (p = 0.005). In addition, plasma Aβ(N-42) levels were also higher in patients that presented multiple lobar macrohemorrhages compared to patients that had one symptomatic hemorrhagic event (p = 0.022), indicating that a certain degree of CAA severity is necessary to show increased Aβ fragments in peripheral circulation., Conclusion: Our results suggest that specific Aβ fragments in plasma might be considered as potential biomarkers for the diagnosis of CAA., (Copyright © 2012 S. Karger AG, Basel.)

Published

2012

27. ACE variants and risk of intracerebral hemorrhage recurrence in amyloid angiopathy.

Author

Domingues-Montanari S, Hernandez-Guillamon M, Fernandez-Cadenas I, Mendioroz M, Boada M, Munuera J, Rovira A, Maisterra O, Parés M, Gutierrez M, Alvarez-Sabin J, Chacón P, Delgado P, and Montaner J

Subjects

Aged, Aged, 80 and over, Analysis of Variance, Apolipoproteins E genetics, Cerebral Amyloid Angiopathy diagnosis, Cerebral Amyloid Angiopathy epidemiology, Cerebral Hemorrhage enzymology, Cerebral Hemorrhage epidemiology, Enzyme-Linked Immunosorbent Assay methods, Female, Genome-Wide Association Study methods, Humans, Kaplan-Meier Estimate, Longitudinal Studies, Magnetic Resonance Imaging, Male, Middle Aged, Peptidyl-Dipeptidase A blood, Recurrence, Risk Factors, Cerebral Amyloid Angiopathy complications, Cerebral Amyloid Angiopathy genetics, Cerebral Hemorrhage etiology, Cerebral Hemorrhage genetics, Peptidyl-Dipeptidase A genetics, Polymorphism, Genetic genetics

Abstract

Cerebral amyloid angiopathy (CAA) is a well-established cause of lobar intracerebral hemorrhage (ICH). The aim of the authors was to investigate the influence of clinical characteristics and genetic variants in the ACE, LRP, MMP9, Tafi, VEGFA, CYP11B2, A2M and APOE on ICH recurrence in a cohort of CAA-related ICH patients. Sixty patients were enrolled and new symptomatic ICHs in the 36 mo following the index event were recorded. Leukoaraiosis degree, microbleeds count and variants in the APOE and ACE were associated with ICH recurrence. The rs4311 variant of the ACE was an independent risk factor (p = 0.001), resisting Bonferroni correction. Moreover, carriers of ε2 of the APOE and TT of the rs4311 of the ACE reached 100% recurrence before 18 mo (p < 0.001). Finally, ACE protein level was measured in serum of controls and depended on the rs4311 genotypes, TT carriers presenting higher level than CC carriers (p = 0.012). These results suggest that variants in the ACE are associated with CAA-related ICH recurrence, possibly by modulating ACE protein level., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published

2011

28. Mobilization, endothelial differentiation and functional capacity of endothelial progenitor cells after ischemic stroke.

Author

Navarro-Sobrino M, Rosell A, Hernandez-Guillamon M, Penalba A, Ribó M, Alvarez-Sabín J, and Montaner J

Subjects

Angiogenic Proteins genetics, Angiogenic Proteins metabolism, Biomarkers metabolism, Brain Ischemia complications, Brain Ischemia drug therapy, Brain Ischemia physiopathology, Case-Control Studies, Cells, Cultured, Endothelial Cells drug effects, Endothelial Cells metabolism, Enzyme-Linked Immunosorbent Assay, Fibrinolytic Agents administration & dosage, Flow Cytometry, Humans, Immunophenotyping, Neovascularization, Physiologic, Phenotype, Polymerase Chain Reaction, RNA, Messenger metabolism, Spain, Stem Cells drug effects, Stem Cells metabolism, Stroke drug therapy, Stroke etiology, Stroke physiopathology, Thrombolytic Therapy, Tissue Plasminogen Activator administration & dosage, Treatment Outcome, Brain Ischemia pathology, Cell Differentiation drug effects, Cell Movement drug effects, Endothelial Cells pathology, Stem Cells pathology, Stroke pathology

Abstract

Endothelial progenitor cells (EPCs) have introduced new possibilities for cell-based vasculogenesis treatment after stroke. In this study we quantified circulating levels of EPCs in stroke patients and in healthy controls, and evaluated the potential of EPCs to induce vasculogenesis in vitro. Blood was drawn from tPA-treated stroke patients and control subjects, and the circulating EPCs levels in each group were quantified by flow cytometry and cell culture assays. Immunophenotyping was performed using multiple markers (UEA-lectin, CD133, vWF and KDR) and tubulogenic function was assessed with the Matrigel® assay. The produced angiogenic factors were quantified by multiple ELISA and RT-PCR. Fluorescence-activated cell sorting (FACS) revealed higher levels of circulating CD133+/CD34+/KDR+/CD45+ cells in the acute strokes as compared to the control subjects (p=0.02). On the other hand, more EPCs grew in cell culture from subacute strokes (p=0.016) than from controls. The endothelial and progenitor lineages of the EPCs were confirmed by immunophenotyping. Interestingly, the appearance of outgrowth EPCs (OECs) correlated positively to stroke severity (p=0.013). Finally, greater capacity to induce vasculogenesis in vitro was found in EPCs from subacute strokes (p=0.03), which we attribute to a higher expression and secretion of angiogenic factors. Our results suggest an early EPC mobilization but an enhanced angiogenic function in the subacute phase of stroke. Nonetheless, development of cell-based therapy for stroke will require further studies to identify those EPCs with the greatest therapeutic potential., (Copyright © 2010 Elsevier Inc. All rights reserved.)

Published

2010

29. Matrix metalloproteinase 2 (MMP-2) degrades soluble vasculotropic amyloid-beta E22Q and L34V mutants, delaying their toxicity for human brain microvascular endothelial cells.

Author

Hernandez-Guillamon M, Mawhirt S, Fossati S, Blais S, Pares M, Penalba A, Boada M, Couraud PO, Neubert TA, Montaner J, Ghiso J, and Rostagno A

Subjects

Amyloid beta-Peptides genetics, Amyloid beta-Peptides metabolism, Blood-Brain Barrier drug effects, Blood-Brain Barrier enzymology, Brain pathology, Endothelial Cells pathology, Gene Expression Regulation, Enzymologic drug effects, Gene Expression Regulation, Enzymologic genetics, Gene Silencing, Humans, Intracranial Hemorrhages enzymology, Intracranial Hemorrhages metabolism, Intracranial Hemorrhages pathology, Matrix Metalloproteinase 2 genetics, Mutation, Missense, Peptides genetics, Peptides metabolism, Amino Acid Substitution, Amyloid beta-Peptides pharmacology, Brain enzymology, Endothelial Cells enzymology, Matrix Metalloproteinase 2 biosynthesis, Peptides pharmacokinetics

Abstract

Patients carrying mutations within the amyloid-beta (Abeta) sequence develop severe early-onset cerebral amyloid angiopathy with some of the related variants manifesting primarily with hemorrhagic phenotypes. Matrix metalloproteases (MMPs) are typically associated with blood brain barrier disruption and hemorrhagic transformations after ischemic stroke. However, their contribution to cerebral amyloid angiopathy-related hemorrhage remains unclear. Human brain endothelial cells challenged with Abeta synthetic homologues containing mutations known to be associated in vivo with hemorrhagic manifestations (AbetaE22Q and AbetaL34V) showed enhanced production and activation of MMP-2, evaluated via Multiplex MMP antibody arrays, gel zymography, and Western blot, which in turn proteolytically cleaved in situ the Abeta peptides. Immunoprecipitation followed by mass spectrometry analysis highlighted the generation of specific C-terminal proteolytic fragments, in particular the accumulation of Abeta-(1-16), a result validated in vitro with recombinant MMP-2 and quantitatively evaluated using deuterium-labeled internal standards. Silencing MMP-2 gene expression resulted in reduced Abeta degradation and enhanced apoptosis. Secretion and activation of MMP-2 as well as susceptibility of the Abeta peptides to MMP-2 degradation were dependent on the peptide conformation, with fibrillar elements of AbetaE22Q exhibiting negligible effects. Our results indicate that MMP-2 release and activation differentially degrades Abeta species, delaying their toxicity for endothelial cells. However, taking into consideration MMP ability to degrade basement membrane components, these protective effects might also undesirably compromise blood brain barrier integrity and precipitate a hemorrhagic phenotype.

Published

2010

30. Plasma VAP-1/SSAO activity predicts intracranial hemorrhages and adverse neurological outcome after tissue plasminogen activator treatment in stroke.

Author

Hernandez-Guillamon M, Garcia-Bonilla L, Solé M, Sosti V, Parés M, Campos M, Ortega-Aznar A, Domínguez C, Rubiera M, Ribó M, Quintana M, Molina CA, Alvarez-Sabín J, Rosell A, Unzeta M, and Montaner J

Subjects

Aged, Aged, 80 and over, Animals, Biomarkers blood, Enzyme Activation drug effects, Enzyme Activation physiology, Female, Humans, Intracranial Hemorrhages drug therapy, Intracranial Hemorrhages etiology, Male, Middle Aged, Nervous System Diseases drug therapy, Nervous System Diseases etiology, Predictive Value of Tests, Prospective Studies, Rats, Rats, Sprague-Dawley, Stroke complications, Stroke drug therapy, Treatment Outcome, Amine Oxidase (Copper-Containing) blood, Cell Adhesion Molecules blood, Intracranial Hemorrhages enzymology, Nervous System Diseases enzymology, Stroke enzymology, Tissue Plasminogen Activator adverse effects

Abstract

Background and Purpose: Vascular adhesion protein-1 (VAP-1) is a cell surface and circulating enzyme involved in recruitment of lymphocytes and neutrophils through its semicarbazide-sensitive amine oxidase (SSAO) activity. We aimed to study plasma VAP-1/SSAO activity in relation to the risk for intracranial bleeding complications in patients with stroke treated with tissue plasminogen activator (tPA), the greatest safety concern with this treatment., Methods: In 141 patients with ischemic stroke, we measured VAP-1/SSAO activity in plasma taken before tPA administration. Hemorrhagic events were classified according to brain CT criteria and functional outcomes evaluated using the National Institutes of Health Stroke Scale. We also assessed the potential therapeutic effect of blocking VAP-1/SSAO activity in a rat embolic stroke model treated with tPA., Results: We saw significantly higher levels of plasma VAP-1/SSAO activity in patients who subsequently experienced hemorrhagic transformation. Elevated plasma VAP-1/SSAO activity also predicted worse neurological outcome in these patients. In the rat model, we confirmed that use of the inhibitor semicarbazide prevented adverse effects caused by delayed tPA administration, leading to a smaller infarct volume., Conclusions: Our data demonstrate that baseline VAP-1/SSAO activity predicts parenchymal hemorrhage after tPA, suggesting the safety of thrombolytic agents could be improved by considering VAP-1/SSAO activity. Furthermore, anti-VAP-1/SSAO drugs given with tPA may prevent neurological worsening in patients with ischemic stroke.

Published

2010

31. p53 phosphorylation is involved in vascular cell death induced by the catalytic activity of membrane-bound SSAO/VAP-1.

Author

Solé M, Hernandez-Guillamon M, Boada M, and Unzeta M

Subjects

Animals, Aorta, Thoracic cytology, Blotting, Western, Caspase 3 metabolism, Cells, Cultured, Mitochondria metabolism, Muscle, Smooth, Vascular metabolism, Phosphorylation drug effects, Proto-Oncogene Proteins c-bcl-2 metabolism, Rats, Transfection, bcl-2-Associated X Protein metabolism, Amine Oxidase (Copper-Containing) genetics, Apoptosis drug effects, Cell Membrane metabolism, Gene Expression Regulation, Enzymologic physiology, Methylamines pharmacology, Muscle, Smooth, Vascular pathology, Tumor Suppressor Protein p53 metabolism

Abstract

Semicarbazide sensitive amine oxidase (SSAO) is a multifunctional enzyme present mainly in adipocytes, endothelial and smooth muscle cells. It metabolizes primary aliphatic and aromatic amines generating products able to contribute to cellular oxidative stress. SSAO is expressed in a membrane-bound form and is also present as a soluble enzyme in plasma. Both isoforms are increased in several pathologies, and the catalytic products generated by the soluble enzymatic activity can induce cytotoxicity of vascular cells in culture. We have analyzed whether the transmembrane form of the enzyme is able to produce a cytotoxic effect through methylamine oxidation. Since cells in culture lose the expression of this enzyme, we used an SSAO stably transfected smooth muscle cell line. Herein we report that cell treatment with the substrate methylamine induced a dose and time dependent cytotoxic effect. The tumor suppressor protein p53 played an important role in the molecular pathway involved in this cell death. Moreover, we also observed the induction of PUMA-alpha expression with mitochondrial Bcl-2 family proteins being affected, and final effector caspases being activated.

Published

2008