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1. Epigenetic regulation by polycomb repressive complex 1 promotes cerebral cavernous malformations

Author

Pham, Van-Cuong, Rödel, Claudia Jasmin, Valentino, Mariaelena, Malinverno, Matteo, Paolini, Alessio, Münch, Juliane, Pasquier, Candice, Onyeogaziri, Favour C, Lazovic, Bojana, Girard, Romuald, Koskimäki, Janne, Hußmann, Melina, Keith, Benjamin, Jachimowicz, Daniel, Kohl, Franziska, Hagelkruys, Astrid, Penninger, Josef M, Schulte-Merker, Stefan, Awad, Issam A, Hicks, Ryan, Magnusson, Peetra U, Faurobert, Eva, Pagani, Massimiliano, and Abdelilah-Seyfried, Salim

Published
2024
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2. Role of Rho-Associated Kinase in the Pathophysiology of Cerebral Cavernous Malformations.

Author

Morrison, Leslie, Liao, James, Gutierrez, Juan, Lopez-Toledano, Miguel, Carrazana, Enrique, Rabinowicz, Adrian, Awad, Issam, Ayata, Cenk, and Kim, Helen

Abstract

Cerebral cavernous malformations (CCMs) are vascular lesions characterized by a porous endothelium. The lack of a sufficient endothelial barrier can result in microbleeds and frank intracerebral hemorrhage. A primary mechanism for lesion development is a sequence variant in at least 1 of the 3 CCM genes (CCM1, CCM2, and CCM3), which influence various signaling pathways that lead to the CCM phenotype. A common downstream process associated with CCM gene loss of function involves overactivation of RhoA and its effector Rho-associated kinase (ROCK). In this study, we review RhoA/ROCK-related mechanisms involved in CCM pathophysiology as potential therapeutic targets. Literature searches were conducted in PubMed using combinations of search terms related to RhoA/ROCK and CCMs. In endothelial cells, CCM1, CCM2, and CCM3 proteins normally associate to form the CCM protein complex, which regulates the functions of a wide variety of protein targets (e.g., MAP3K3, SMURF1, SOK-1, and ICAP-1) that directly or indirectly increase RhoA/ROCK activity. Loss of CCM complex function and increased RhoA/ROCK activity can lead to the formation of stress fibers that contribute to endothelial junction instability. Other RhoA/ROCK-mediated pathophysiologic outcomes include a shift to a senescence-associated secretory phenotype (primarily mediated by ROCK2), which is characterized by endothelial cell migration, cell cycle arrest, extracellular matrix degradation, leukocyte chemotaxis, and inflammation. ROCK represents a potential therapeutic target, and direct (fasudil, NRL-1049) and indirect (statins) ROCK inhibitors have demonstrated various levels of efficacy in reducing lesion burden in preclinical models of CCM. Current (atorvastatin) and planned (NRL-1049) clinical studies will determine the efficacy of ROCK inhibitors for CCM in humans, for which no US Food and Drug Administration-approved or EU-approved pharmacologic treatment exists.

Published
2024

3. Transcriptomic signatures of individual cell types in cerebral cavernous malformation

Author

Li, Ying, Girard, Romuald, Srinath, Abhinav, Cruz, Diana Vera, Ciszewski, Cezary, Chen, Chang, Lightle, Rhonda, Romanos, Sharbel, Sone, Je Yeong, Moore, Thomas, DeBiasse, Dorothy, Stadnik, Agnieszka, Lee, Justine J., Shenkar, Robert, Koskimäki, Janne, Lopez-Ramirez, Miguel A., Marchuk, Douglas A., Ginsberg, Mark H., Kahn, Mark L., Shi, Changbin, and Awad, Issam A.

Published
2024
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4. Trial Readiness of Cavernous Malformations With Symptomatic Hemorrhage, Part II: Biomarkers and Trial Modeling.

Author

Hage, Stephanie, Kinkade, Serena, Girard, Romuald, Flemming, Kelly, Kim, Helen, Torbey, Michel, Huang, Judy, Huston, John, Shu, Yunhong, Selwyn, Reed, Hart, Blaine, Mabray, Marc, Feghali, James, Sair, Haris, Narvid, Jared, Lupo, Janine, Lee, Justine, Stadnik, Agnieszka, Alcazar-Felix, Roberto, Shenkar, Robert, Hobson, Nicholas, DeBiasse, Dorothy, Lane, Karen, McBee, Nichole, Treine, Kevin, Ostapkovich, Noeleen, Wang, Ying, Thompson, Richard, Koenig, James, Carroll, Timothy, Hanley, Daniel, and Awad, Issam

Subjects
biomarkers, hemorrhage, iron, perfusion, permeability, Humans, Prospective Studies, Hemorrhage, Hemangioma, Cavernous, Central Nervous System, Biomarkers, Magnetic Resonance Imaging, Cerebral Hemorrhage
Abstract

BACKGROUND: Quantitative susceptibility mapping (QSM) and dynamic contrast-enhanced quantitative perfusion (DCEQP) magnetic resonance imaging sequences assessing iron deposition and vascular permeability were previously correlated with new hemorrhage in cerebral cavernous malformations. We assessed their prospective changes in a multisite trial-readiness project. METHODS: Patients with cavernous malformation and symptomatic hemorrhage (SH) in the prior year, without prior or planned lesion resection or irradiation were enrolled. Mean QSM and DCEQP of the SH lesion were acquired at baseline and at 1- and 2-year follow-ups. Sensitivity and specificity of biomarker changes were analyzed in relation to predefined criteria for recurrent SH or asymptomatic change. Sample size calculations for hypothesized therapeutic effects were conducted. RESULTS: We logged 143 QSM and 130 DCEQP paired annual assessments. Annual QSM change was greater in cases with SH than in cases without SH (P=0.019). Annual QSM increase by ≥6% occurred in 7 of 7 cases (100%) with recurrent SH and in 7 of 10 cases (70%) with asymptomatic change during the same epoch and 3.82× more frequently than clinical events. DCEQP change had lower sensitivity for SH and asymptomatic change than QSM change and greater variance. A trial with the smallest sample size would detect a 30% difference in QSM annual change during 2 years of follow-up in 34 or 42 subjects (1 and 2 tailed, respectively); power, 0.8, α=0.05. CONCLUSIONS: Assessment of QSM change is feasible and sensitive to recurrent bleeding in cavernous malformations. Evaluation of an intervention on QSM percent change may be used as a time-averaged difference between 2 arms using a repeated measures analysis. DCEQP change is associated with lesser sensitivity and higher variability than QSM. These results are the basis of an application for certification by the US Food and Drug Administration of QSM as a biomarker of drug effect on bleeding in cavernous malformations. REGISTRATION: URL: https://www.clinicaltrials.gov; Unique identifier: NCT03652181.

Published
2024

5. Trial Readiness of Cavernous Malformations With Symptomatic Hemorrhage, Part I: Event Rates and Clinical Outcome.

Author

Flemming, Kelly, Kim, Helen, Hage, Stephanie, Mandrekar, Jay, Kinkade, Serena, Girard, Romuald, Torbey, Michel, Huang, Judy, Huston, John, Shu, Yunhong, Lanzino, Giuseppe, Selwyn, Reed, Hart, Blaine, Mabray, Marc, Feghali, James, Sair, Haris, Narvid, Jared, Lupo, Janine, Lee, Justine, Stadnik, Agnieszka, Alcazar-Felix, Roberto, Shenkar, Robert, Lane, Karen, McBee, Nichole, Treine, Kevin, Ostapkovich, Noeleen, Wang, Ying, Thompson, Richard, Koenig, James, Carroll, Timothy, Hanley, Daniel, and Awad, Issam

Subjects
cavernous angioma, intracranial hemorrhage, patient-reported outcome, quality of life, trial readiness, Adult, Humans, Hemangioma, Cavernous, Central Nervous System, Hemorrhage, Prospective Studies, Quality of Life, Stroke, Treatment Outcome
Abstract

BACKGROUND: Cerebral cavernous malformation with symptomatic hemorrhage (SH) are targets for novel therapies. A multisite trial-readiness project (https://www.clinicaltrials.gov; Unique identifier: NCT03652181) aimed to identify clinical, imaging, and functional changes in these patients. METHODS: We enrolled adult cerebral cavernous malformation patients from 5 high-volume centers with SH within the prior year and no planned surgery. In addition to clinical and imaging review, we assessed baseline, 1- and 2-year National Institutes of Health Stroke Scale, modified Rankin Scale, European Quality of Life 5D-3 L, and patient-reported outcome-measurement information system, Version 2.0. SH and asymptomatic change rates were adjudicated. Changes in functional scores were assessed as a marker for hemorrhage. RESULTS: One hundred twenty-three, 102, and 69 patients completed baseline, 1- and 2-year clinical assessments, respectively. There were 21 SH during 178.3 patient years of follow-up (11.8% per patient year). At baseline, 62.6% and 95.1% of patients had a modified Rankin Scale score of 1 and National Institutes of Health Stroke Scale score of 0 to 4, respectively, which improved to 75.4% (P=0.03) and 100% (P=0.06) at 2 years. At baseline, 74.8% had at least one abnormal patient-reported outcome-measurement information system, Version 2.0 domain compared with 61.2% at 2 years (P=0.004). The most common abnormal European Quality of Life 5D-3 L domains were pain (48.7%), anxiety (41.5%), and participation in usual activities (41.4%). Patients with prospective SH were more likely than those without SH to display functional decline in sleep, fatigue, and social function patient-reported outcome-measurement information system, Version 2.0 domains at 2 years. Other score changes did not differ significantly between groups at 2 years. The sensitivity of scores as an SH marker remained poor at the time interval assessed. CONCLUSIONS: We report SH rate, functional, and patient-reported outcomes in trial-eligible cerebral cavernous malformation with SH patients. Functional outcomes and patient-reported outcomes generally improved over 2 years. No score change was highly sensitive or specific for SH and could not be used as a primary end point in a trial.

Published
2024

6. Except for Robust Outliers, Rapamycin Increases Lesion Burden in a Murine Model of Cerebral Cavernous Malformations

Author

Alcazar-Felix, Roberto J., Shenkar, Robert, Benavides, Christian R., Bindal, Akash, Srinath, Abhinav, Li, Ying, Kinkade, Serena, Terranova, Tatiana, DeBose-Scarlett, Evon, Lightle, Rhonda, DeBiasse, Dorothy, Almazroue, Hanadi, Cruz, Diana Vera, Romanos, Sharbel, Jhaveri, Aditya, Koskimäki, Janne, Hage, Stephanie, Bennett, Carolyn, Girard, Romuald, Marchuk, Douglas A., and Awad, Issam A.

Published
2024
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9. Plasma metabolites with mechanistic and clinical links to the neurovascular disease cavernous angioma

Author

Srinath, Abhinav, Xie, Bingqing, Li, Ying, Sone, Je Yeong, Romanos, Sharbel, Chen, Chang, Sharma, Anukriti, Polster, Sean, Dorrestein, Pieter C, Weldon, Kelly C, DeBiasse, Dorothy, Moore, Thomas, Lightle, Rhonda, Koskimäki, Janne, Zhang, Dongdong, Stadnik, Agnieszka, Piedad, Kristina, Hagan, Matthew, Shkoukani, Abdallah, Carrión-Penagos, Julián, Bi, Dehua, Shen, Le, Shenkar, Robert, Ji, Yuan, Sidebottom, Ashley, Pamer, Eric, Gilbert, Jack A, Kahn, Mark L, D’Souza, Mark, Sulakhe, Dinanath, Awad, Issam A, and Girard, Romuald

Subjects
Brain Disorders, Genetics, Rare Diseases, Neurosciences
Abstract

BackgroundCavernous angiomas (CAs) affect 0.5% of the population, predisposing to serious neurologic sequelae from brain bleeding. A leaky gut epithelium associated with a permissive gut microbiome, was identified in patients who develop CAs, favoring lipid polysaccharide producing bacterial species. Micro-ribonucleic acids along with plasma levels of proteins reflecting angiogenesis and inflammation were also previously correlated with CA and CA with symptomatic hemorrhage.MethodsThe plasma metabolome of CA patients and CA patients with symptomatic hemorrhage was assessed using liquid-chromatography mass spectrometry. Differential metabolites were identified using partial least squares-discriminant analysis (p

Published
2023

10. Circulating Plasma miRNA Homologs in Mice and Humans Reflect Familial Cerebral Cavernous Malformation Disease

Author

Romanos, Sharbel G., Srinath, Abhinav, Li, Ying, Xie, Bingqing, Chen, Chang, Li, Yan, Moore, Thomas, Bi, Dehua, Sone, Je Yeong, Lightle, Rhonda, Hobson, Nick, Zhang, Dongdong, Koskimäki, Janne, Shen, Le, McCurdy, Sara, Lai, Catherine Chinhchu, Stadnik, Agnieszka, Piedad, Kristina, Carrión-Penagos, Julián, Shkoukani, Abdallah, Snellings, Daniel, Shenkar, Robert, Sulakhe, Dinanath, Ji, Yuan, Lopez-Ramirez, Miguel A., Kahn, Mark L., Marchuk, Douglas A., Ginsberg, Mark H., Girard, Romuald, and Awad, Issam A.

Published
2023
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11. Mild Hypoxia Accelerates Cerebral Cavernous Malformation Disease Through CX3CR1-CX3CL1 Signaling

Author

Frias-Anaya, Eduardo, Gallego-Gutierrez, Helios, Gongol, Brendan, Weinsheimer, Shantel, Lai, Catherine Chinhchu, Orecchioni, Marco, Sriram, Aditya, Bui, Cassandra M., Nelsen, Bliss, Hale, Preston, Pham, Angela, Shenkar, Robert, DeBiasse, Dorothy, Lightle, Rhonda, Girard, Romuald, Li, Ying, Srinath, Abhinav, Daneman, Richard, Nudleman, Eric, Sun, Hao, Guma, Monica, Dubrac, Alexandre, Mesarwi, Omar A., Ley, Klaus, Kim, Helen, Awad, Issam A., Ginsberg, Mark H., and Lopez-Ramirez, Miguel Alejandro

Published
2024
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13. Baseline Characteristics of Patients With Cavernous Angiomas With Symptomatic Hemorrhage in Multisite Trial Readiness Project

Author

Kim, Helen, Flemming, Kelly D, Nelson, Jeffrey A, Lui, Avery, Majersik, Jennifer J, Dela Cruz, Michael, Zabramski, Joseph, Trevizo, Odilette, Lanzino, Giuseppe, Zafar, Atif, Torbey, Michel, Mabray, Marc C, Robinson, Myranda, Narvid, Jared, Lupo, Janine, Thompson, Richard E, Hanley, Daniel F, McBee, Nichol, Treine, Kevin, Ostapkovich, Noeleen, Stadnik, Agnieszka, Piedad, Kristina, Hobson, Nicholas, Carroll, Timothy, Shkoukani, Abdallah, Carrión-Penagos, Julián, Mendoza-Puccini, Carolina, Koenig, James I, and Awad, Issam

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Clinical Research, Clinical Trials and Supportive Activities, Neurosciences, Stroke, Brain Disorders, Good Health and Well Being, Adult, Aged, Brain Neoplasms, Cerebral Hemorrhage, Cohort Studies, Female, Hemangioma, Cavernous, Central Nervous System, Humans, Magnetic Resonance Imaging, Male, Middle Aged, Neuroimaging, biomarkers, clinical trial, intracranial hemorrhage, magnetic resonance imaging, quality of life, vascular malformations, Cardiorespiratory Medicine and Haematology, Neurology & Neurosurgery, Clinical sciences, Allied health and rehabilitation science
Abstract

Background and purposeBrain cavernous angiomas with symptomatic hemorrhage (CASH) have a high risk of neurological disability from recurrent bleeding. Systematic assessment of baseline features and multisite validation of novel magnetic resonance imaging biomarkers are needed to optimize clinical trial design aimed at novel pharmacotherapies in CASH.MethodsThis prospective, multicenter, observational cohort study included adults with unresected, adjudicated brain CASH within the prior year. Six US sites screened and enrolled patients starting August 2018. Baseline demographics, clinical and imaging features, functional status (modified Rankin Scale and National Institutes of Health Stroke Scale), and patient quality of life outcomes (Patient-Reported Outcomes Measurement Information System-29 and EuroQol-5D) were summarized using descriptive statistics. Patient-Reported Outcomes Measurement Information System-29 scores were standardized against a reference population (mean 50, SD 10), and one-sample t test was performed for each domain. A subgroup underwent harmonized magnetic resonance imaging assessment of lesional iron content with quantitative susceptibility mapping and vascular permeability with dynamic contrast-enhanced quantitative perfusion.ResultsAs of May 2020, 849 patients were screened and 110 CASH cases enrolled (13% prevalence of trial eligible cases). The average age at consent was 46±16 years, 53% were female, 41% were familial, and 43% were brainstem lesions. At enrollment, ≥90% of the cohort had independent functional outcome (modified Rankin Scale score ≤2 and National Institutes of Health Stroke Scale score 30% of patients (EuroQol-5D). Patients had significantly worse Patient-Reported Outcomes Measurement Information System-29 scores for anxiety (P=0.007), but better depression (P=0.002) and social satisfaction scores (P=0.012) compared with the general reference population. Mean baseline quantitative susceptibility mapping and permeability of CASH lesion were 0.45±0.17 ppm and 0.39±0.31 mL/100 g per minute, respectively, which were similar to historical CASH cases and consistent across sites.ConclusionsThese baseline features will aid investigators in patient stratification and determining the most appropriate outcome measures for clinical trials of emerging pharmacotherapies in CASH.

Published
2021

15. A Roadmap for Developing Plasma Diagnostic and Prognostic Biomarkers of Cerebral Cavernous Angioma With Symptomatic Hemorrhage (CASH)

Author

Girard, Romuald, Li, Yan, Stadnik, Agnieszka, Shenkar, Robert, Hobson, Nicholas, Romanos, Sharbel, Srinath, Abhinav, Moore, Thomas, Lightle, Rhonda, Shkoukani, Abdallah, Akers, Amy, Carroll, Timothy, Christoforidis, Gregory A, Koenig, James I, Lee, Cornelia, Piedad, Kristina, Greenberg, Steven M, Kim, Helen, Flemming, Kelly D, Ji, Yuan, and Awad, Issam A

Subjects
Reproductive Medicine, Biomedical and Clinical Sciences, Rare Diseases, Neurosciences, Prevention, Brain Disorders, Detection, screening and diagnosis, 4.1 Discovery and preclinical testing of markers and technologies, 4.2 Evaluation of markers and technologies, Cardiovascular, Good Health and Well Being, Biomarkers, Brain Neoplasms, Capillary Permeability, Cerebral Hemorrhage, Female, Hemangioma, Cavernous, Hemangioma, Cavernous, Central Nervous System, Humans, Inflammation Mediators, Longitudinal Studies, Machine Learning, Magnetic Resonance Imaging, Male, Prognosis, Transcriptome, Cavernous angioma with symptomatic hemorrhage, Cavernous angioma, Cerebral cavernous malformation, Symptomatic hemorrhage, Machine learning, Plasma, QSM, Clinical Sciences, Neurology & Neurosurgery, Clinical sciences, Biological psychology
Abstract

BackgroundCerebral cavernous angioma (CA) is a capillary microangiopathy predisposing more than a million Americans to premature risk of brain hemorrhage. CA with recent symptomatic hemorrhage (SH), most likely to re-bleed with serious clinical sequelae, is the primary focus of therapeutic development. Signaling aberrations in CA include proliferative dysangiogenesis, blood-brain barrier hyperpermeability, inflammatory/immune processes, and anticoagulant vascular domain. Plasma levels of molecules reflecting these mechanisms and measures of vascular permeability and iron deposition on magnetic resonance imaging are biomarkers that have been correlated with CA hemorrhage.ObjectiveTo optimize these biomarkers to accurately diagnose cavernous angioma with symptomatic hemorrhage (CASH), prognosticate the risk of future SH, and monitor cases after a bleed and in response to therapy.MethodsAdditional candidate biomarkers, emerging from ongoing mechanistic and differential transcriptome studies, would further enhance the sensitivity and specificity of diagnosis and prediction of CASH. Integrative combinations of levels of plasma proteins and characteristic micro-ribonucleic acids may further strengthen biomarker associations. We will deploy advanced statistical and machine learning approaches for the integration of novel candidate biomarkers, rejecting noncorrelated candidates, and determining the best clustering and weighing of combined biomarker contributions.Expected outcomesWith the expertise of leading CA researchers, this project anticipates the development of future blood tests for the diagnosis and prediction of CASH to clinically advance towards precision medicine.DiscussionThe project tests a novel integrational approach of biomarker development in a mechanistically defined cerebrovascular disease with a relevant context of use, with an approach applicable to other neurological diseases with similar pathobiologic features.

Published
2021

17. Permissive microbiome characterizes human subjects with a neurovascular disease cavernous angioma.

Author

Polster, Sean P, Sharma, Anukriti, Tanes, Ceylan, Tang, Alan T, Mericko, Patricia, Cao, Ying, Carrión-Penagos, Julián, Girard, Romuald, Koskimäki, Janne, Zhang, Dongdong, Stadnik, Agnieszka, Romanos, Sharbel G, Lyne, Seán B, Shenkar, Robert, Yan, Kimberly, Lee, Cornelia, Akers, Amy, Morrison, Leslie, Robinson, Myranda, Zafar, Atif, Bittinger, Kyle, Kim, Helen, Gilbert, Jack A, Kahn, Mark L, Shen, Le, and Awad, Issam A

Abstract

Cavernous angiomas (CA) are common vascular anomalies causing brain hemorrhage. Based on mouse studies, roles of gram-negative bacteria and altered intestinal homeostasis have been implicated in CA pathogenesis, and pilot study had suggested potential microbiome differences between non-CA and CA individuals based on 16S rRNA gene sequencing. We here assess microbiome differences in a larger cohort of human subjects with and without CA, and among subjects with different clinical features, and conduct more definitive microbial analyses using metagenomic shotgun sequencing. Relative abundance of distinct bacterial species in CA patients is shown, consistent with postulated permissive microbiome driving CA lesion genesis via lipopolysaccharide signaling, in humans as in mice. Other microbiome differences are related to CA clinical behavior. Weighted combinations of microbiome signatures and plasma inflammatory biomarkers enhance associations with disease severity and hemorrhage. This is the first demonstration of a sensitive and specific diagnostic microbiome in a human neurovascular disease.

Published
2020

20. Safety and efficacy of propranolol for treatment of familial cerebral cavernous malformations (Treat_CCM): a randomised, open-label, blinded-endpoint, phase 2 pilot trial

Author

Abete Fornara, Giorgia, Agnelli, Nicolò M., Albanese, Alessio, Awad, Issam, Bagnati, Renzo, Balconi, Giovanna, Ballabio, Elena, Beghi, Ettore, Bernasconi, Roberto, Bertani, Giulio A., Besana, Silvia, Blanda, Adriana, Bossi, Chiara, Bresolin, Nereo, Buratti, Maria G., Calabrese, Roberta, Carriero, Maria R., Castori, Marco, Ciceri, Elisa F., Ciurleo, Rossella, Comi, Giacomo P., Contarino, Valeria, Conte, Giorgio, D'Agruma, Leonardo, D'Alessandris, Giorgio Q., de Grazia, Ugo, Di Bonaventura, Rina, d'Orio, Piergiorgio, Farago', Giuseppe, Foresta, Andreana, Fusco, Carmela, Gaudino, Chiara, Lampugnani, Maria G., Lanno, Alessia, Lazzaroni, Francesca, Lee, Cornelia, Locatelli, Marco, Maggioni, Aldo P., Magnusson, Peetra, Malinverno, Matteo, Mangiavacchi, Maurizio, Mangraviti, Antonella, Marino, Silvia, Mazzola, Selene, Nicolis, Enrico B., Novelli, Deborah, Ojeda Fernandez, Maria L., Petracca, Antonio, Pignotti, Fabrizio, Pogliani, Simona, Poloni, Marco, Prelle, Alessandro, Raggi, Pamela, Raucci, Franca, Regna-Gladin, Caroline, Ronchi, Dario, Scelzo, Emma, Seyfried, Salim, Simeone, Anna, Sturiale, Carmelo L., Tassi, Laura, Tettamanti, Mauro, Torri, Valter, Tournier-Lasserve, Elisabeth, Treglia, Rita, Triulzi, Fabio M., Ungaro, Celeste, Ursi, Elison, Valcamonica, Gloria, Vasami', Antonella, Zarino, Barbara, Lanfranconi, Silvia, Scola, Elisa, Meessen, Jennifer M T A, Pallini, Roberto, Bertani, Giulio A, Al-Shahi Salman, Rustam, Dejana, Elisabetta, and Latini, Roberto

Published
2023
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21. Distinct cellular roles for PDCD10 define a gut-brain axis in cerebral cavernous malformation

Author

Tang, Alan T, Sullivan, Katie R, Hong, Courtney C, Goddard, Lauren M, Mahadevan, Aparna, Ren, Aileen, Pardo, Heidy, Peiper, Amy, Griffin, Erin, Tanes, Ceylan, Mattei, Lisa M, Yang, Jisheng, Li, Li, Mericko-Ishizuka, Patricia, Shen, Le, Hobson, Nicholas, Girard, Romuald, Lightle, Rhonda, Moore, Thomas, Shenkar, Robert, Polster, Sean P, Rödel, Claudia J, Li, Ning, Zhu, Qin, Whitehead, Kevin J, Zheng, Xiangjian, Akers, Amy, Morrison, Leslie, Kim, Helen, Bittinger, Kyle, Lengner, Christopher J, Schwaninger, Markus, Velcich, Anna, Augenlicht, Leonard, Abdelilah-Seyfried, Salim, Min, Wang, Marchuk, Douglas A, Awad, Issam A, and Kahn, Mark L

Subjects
Rare Diseases, Neurosciences, Genetics, Brain Disorders, Aetiology, 2.1 Biological and endogenous factors, Oral and gastrointestinal, Animals, Apoptosis Regulatory Proteins, Brain, Carrier Proteins, Colitis, Dexamethasone, Dextran Sulfate, Endothelial Cells, Epithelial Cells, Gastrointestinal Microbiome, Gastrointestinal Tract, Hemangioma, Cavernous, Central Nervous System, Humans, Intestinal Mucosa, KRIT1 Protein, Ligands, Membrane Proteins, Mice, Proto-Oncogene Proteins, Signal Transduction, Toll-Like Receptor 4, Biological Sciences, Medical and Health Sciences
Abstract

Cerebral cavernous malformation (CCM) is a genetic, cerebrovascular disease. Familial CCM is caused by genetic mutations in KRIT1, CCM2, or PDCD10 Disease onset is earlier and more severe in individuals with PDCD10 mutations. Recent studies have shown that lesions arise from excess mitogen-activated protein kinase kinase kinase 3 (MEKK3) signaling downstream of Toll-like receptor 4 (TLR4) stimulation by lipopolysaccharide derived from the gut microbiome. These findings suggest a gut-brain CCM disease axis but fail to define it or explain the poor prognosis of patients with PDCD10 mutations. Here, we demonstrate that the gut barrier is a primary determinant of CCM disease course, independent of microbiome configuration, that explains the increased severity of CCM disease associated with PDCD10 deficiency. Chemical disruption of the gut barrier with dextran sulfate sodium augments CCM formation in a mouse model, as does genetic loss of Pdcd10, but not Krit1, in gut epithelial cells. Loss of gut epithelial Pdcd10 results in disruption of the colonic mucosal barrier. Accordingly, loss of Mucin-2 or exposure to dietary emulsifiers that reduce the mucus barrier increases CCM burden analogous to loss of Pdcd10 in the gut epithelium. Last, we show that treatment with dexamethasone potently inhibits CCM formation in mice because of the combined effect of action at both brain endothelial cells and gut epithelial cells. These studies define a gut-brain disease axis in an experimental model of CCM in which a single gene is required for two critical components: gut epithelial function and brain endothelial signaling.

Published
2019

22. Biomarkers of cavernous angioma with symptomatic hemorrhage

Author

Lyne, Seán B, Girard, Romuald, Koskimäki, Janne, Zeineddine, Hussein A, Zhang, Dongdong, Cao, Ying, Li, Yan, Stadnik, Agnieszka, Moore, Thomas, Lightle, Rhonda, Shi, Changbin, Shenkar, Robert, Carrión-Penagos, Julián, Polster, Sean P, Romanos, Sharbel, Akers, Amy, Lopez-Ramirez, Miguel, Whitehead, Kevin J, Kahn, Mark L, Ginsberg, Mark H, Marchuk, Douglas A, and Awad, Issam A

Subjects
Prevention, Clinical Research, Clinical Trials and Supportive Activities, 4.1 Discovery and preclinical testing of markers and technologies, Detection, screening and diagnosis, 4.2 Evaluation of markers and technologies, Good Health and Well Being, Adult, Biomarkers, Cohort Studies, Female, Hemangioma, Cavernous, Hemorrhage, Humans, Inflammation Mediators, Longitudinal Studies, Machine Learning, Male, Transcriptome, Diagnostics, Inflammation, Stroke, Vascular Biology
Abstract

BACKGROUNDCerebral cavernous angiomas (CAs) with a symptomatic hemorrhage (CASH) have a high risk of recurrent hemorrhage and serious morbidity.METHODSEighteen plasma molecules with mechanistic roles in CA pathobiology were investigated in 114 patients and 12 healthy subjects. The diagnostic biomarker of a CASH in the prior year was derived as that minimizing the Akaike information criterion and validated using machine learning, and was compared with the prognostic CASH biomarker predicting bleeding in the subsequent year. Biomarkers were longitudinally followed in a subset of cases. The biomarkers were queried in the lesional neurovascular unit (NVU) transcriptome and in plasma miRNAs from CASH and non-CASH patients.RESULTSThe diagnostic CASH biomarker included a weighted combination of soluble CD14 (sCD14), VEGF, C-reactive protein (CRP), and IL-10 distinguishing CASH patients with 76% sensitivity and 80% specificity (P = 0.0003). The prognostic CASH biomarker (sCD14, VEGF, IL-1β, and sROBO-4) was confirmed to predict a bleed in the subsequent year with 83% sensitivity and 93% specificity (P = 0.001). Genes associated with diagnostic and prognostic CASH biomarkers were differentially expressed in CASH lesional NVUs. Thirteen plasma miRNAs were differentially expressed between CASH and non-CASH patients.CONCLUSIONShared and unique biomarkers of recent symptomatic hemorrhage and of future bleeding in CA are mechanistically linked to lesional transcriptome and miRNA. The biomarkers may be applied for risk stratification in clinical trials and developed as a tool in clinical practice.FUNDINGNIH, William and Judith Davis Fund in Neurovascular Surgery Research, Be Brave for Life Foundation, Safadi Translational Fellowship, Pritzker School of Medicine, and Sigrid Jusélius Foundation.

Published
2019

23. Trial Readiness in Cavernous Angiomas With Symptomatic Hemorrhage (CASH).

Author

Polster, Sean P, Cao, Ying, Carroll, Timothy, Flemming, Kelly, Girard, Romuald, Hanley, Daniel, Hobson, Nicholas, Kim, Helen, Koenig, James, Koskimäki, Janne, Lane, Karen, Majersik, Jennifer J, McBee, Nichol, Morrison, Leslie, Shenkar, Robert, Stadnik, Agnieszka, Thompson, Richard E, Zabramski, Joseph, Zeineddine, Hussein A, and Awad, Issam A

Subjects
Humans, Hemangioma, Cavernous, Central Nervous System, Central Nervous System Neoplasms, Hemorrhage, Cohort Studies, Feasibility Studies, Biomarkers, Cavernous angioma, Cerebral cavernous malformation, Drug development, Symptomatic hemorrhage, Trial readiness, Clinical Trials and Supportive Activities, Stroke, Brain Disorders, Prevention, Neurosciences, Clinical Research, Detection, screening and diagnosis, 4.2 Evaluation of markers and technologies, Clinical Sciences, Neurology & Neurosurgery
Abstract

BACKGROUND:Brain cavernous angiomas with symptomatic hemorrhage (CASH) are uncommon but exact a heavy burden of neurological disability from recurrent bleeding, for which there is no proven therapy. Candidate drugs to stabilize the CASH lesion and prevent rebleeding will ultimately require testing of safety and efficacy in multisite clinical trials. Much progress has been made in understanding the epidemiology of CASH, and novel biomarkers have been linked to the biological mechanisms and clinical activity in lesions. Yet, the ability to enroll and risk-stratify CASH subjects has never been assessed prospectively at multiple sites. Biomarkers and other outcomes have not been evaluated for their sensitivity and reliability, nor have they been harmonized across sites. OBJECTIVE:To address knowledge gaps and establish a research network as infrastructure for future clinical trials, through the Trial Readiness grant mechanism, funded by National Institute of Neurological Disorders and Stroke/National Institutes of Health. METHODS:This project includes an observational cohort study to assess (1) the feasibility of screening, enrollment rates, baseline disease categorization, and follow-up of CASH using common data elements at multiple sites, (2) the reliability of imaging biomarkers including quantitative susceptibility mapping and permeability measures that have been shown to correlate with lesion activity, and (3) the rates of recurrent hemorrhage and change in functional status and biomarker measurements during prospective follow-up. EXPECTED OUTCOMES:We propose a harmonized multisite assessment of enrollment rates of CASH, baseline features relevant to stratification in clinical trials, and follow-up assessments of functional outcomes in relation to clinical bleeds. We introduce novel biomarkers of vascular leak and hemorrhage, with firm mechanistic foundations, which have been linked to clinical disease activity. We shall test their reliability and validity at multiple sites, and assess their changes over time, with and without clinical rebleeds, hence their fitness as outcome instruments in clinical trials. DISCUSSION:The timing cannot be more opportune, with therapeutic targets identified, exceptional collaboration among researchers and the patient community, along with several drugs ready to benefit from development of a path to clinical testing using this network in the next 5 years.

Published
2019

24. Phenotypic characterization of murine models of cerebral cavernous malformations

Author

Zeineddine, Hussein A, Girard, Romuald, Saadat, Laleh, Shen, Le, Lightle, Rhonda, Moore, Thomas, Cao, Ying, Hobson, Nick, Shenkar, Robert, Avner, Kenneth, Chaudager, Kiranj, Koskimäki, Janne, Polster, Sean P, Fam, Maged D, Shi, Changbin, Lopez-Ramirez, Miguel Alejandro, Tang, Alan T, Gallione, Carol, Kahn, Mark L, Ginsberg, Mark, Marchuk, Douglas A, and Awad, Issam A

Subjects
Medical Physiology, Biomedical and Clinical Sciences, Rare Diseases, Neurosciences, Genetics, Brain Disorders, 2.1 Biological and endogenous factors, Aetiology, Cardiovascular, Acute Disease, Animals, Apoptosis Regulatory Proteins, B-Lymphocytes, Brain, Cerebellum, Chronic Disease, Disease Models, Animal, Endothelial Cells, Hemangioma, Cavernous, Central Nervous System, Humans, Intracellular Signaling Peptides and Proteins, Iron, KRIT1 Protein, Mice, Mice, Knockout, Mice, Transgenic, Microfilament Proteins, Mutation, Occludin, Phenotype, T-Lymphocytes, rho-Associated Kinases, Clinical Sciences, Pathology, Clinical sciences
Abstract

Cerebral cavernous malformations (CCMs) are clusters of dilated capillaries that affect around 0.5% of the population. CCMs exist in two forms, sporadic and familial. Mutations in three documented genes, KRIT1(CCM1), CCM2, and PDCD10(CCM3), cause the autosomal dominant form of the disease, and somatic mutations in these same genes underlie lesion development in the brain. Murine models with constitutive or induced loss of respective genes have been applied to study disease pathobiology and therapeutic manipulations. We aimed to analyze the phenotypic characteristic of two main groups of models, the chronic heterozygous models with sensitizers promoting genetic instability, and the acute neonatal induced homozygous knockout model. Acute model mice harbored a higher lesion burden than chronic models, more localized in the hindbrain, and largely lacking iron deposition and inflammatory cell infiltrate. The chronic model mice showed a lower lesion burden localized throughout the brain, with significantly greater perilesional iron deposition, immune B- and T-cell infiltration, and less frequent junctional protein immunopositive endothelial cells. Lesional endothelial cells in both models expressed similar phosphorylated myosin light chain immunopositivity indicating Rho-associated protein kinase activity. These data suggest that acute models are better suited to study the initial formation of the lesion, while the chronic models better reflect lesion maturation, hemorrhage, and inflammatory response, relevant pathobiologic features of the human disease.

Published
2019

25. Comprehensive transcriptome analysis of cerebral cavernous malformation across multiple species and genotypes

Author

Koskimäki, Janne, Girard, Romuald, Li, Yan, Saadat, Laleh, Zeineddine, Hussein A, Lightle, Rhonda, Moore, Thomas, Lyne, Seán, Avner, Kenneth, Shenkar, Robert, Cao, Ying, Shi, Changbin, Polster, Sean P, Zhang, Dongdong, Carrión-Penagos, Julián, Romanos, Sharbel, Fonseca, Gregory, Lopez-Ramirez, Miguel A, Chapman, Eric M, Popiel, Evelyn, Tang, Alan T, Akers, Amy, Faber, Pieter, Andrade, Jorge, Ginsberg, Mark, Derry, W Brent, Kahn, Mark L, Marchuk, Douglas A, and Awad, Issam A

Subjects
Neurosciences, Genetics, Rare Diseases, Brain Disorders, Aetiology, Underpinning research, 2.1 Biological and endogenous factors, 1.1 Normal biological development and functioning, Molecular genetics, Neuroscience, Transcription, Vascular Biology, endothelial cells
Abstract

The purpose of this study was to determine important genes, functions, and networks contributing to the pathobiology of cerebral cavernous malformation (CCM) from transcriptomic analyses across 3 species and 2 disease genotypes. Sequencing of RNA from laser microdissected neurovascular units of 5 human surgically resected CCM lesions, mouse brain microvascular endothelial cells, Caenorhabditis elegans with induced Ccm gene loss, and their respective controls provided differentially expressed genes (DEGs). DEGs from mouse and C. elegans were annotated into human homologous genes. Cross-comparisons of DEGs between species and genotypes, as well as network and gene ontology (GO) enrichment analyses, were performed. Among hundreds of DEGs identified in each model, common genes and 1 GO term (GO:0051656, establishment of organelle localization) were commonly identified across the different species and genotypes. In addition, 24 GO functions were present in 4 of 5 models and were related to cell-to-cell adhesion, neutrophil-mediated immunity, ion transmembrane transporter activity, and responses to oxidative stress. We have provided a comprehensive transcriptome library of CCM disease across species and for the first time to our knowledge in Ccm1/Krit1 versus Ccm3/Pdcd10 genotypes. We have provided examples of how results can be used in hypothesis generation or mechanistic confirmatory studies.

Published
2019

30. Thrombospondin1 (TSP1) replacement prevents cerebral cavernous malformations

Author

Lopez-Ramirez, Miguel Alejandro, Fonseca, Gregory, Zeineddine, Hussein A, Girard, Romuald, Moore, Thomas, Pham, Angela, Cao, Ying, Shenkar, Robert, de Kreuk, Bart-Jan, Lagarrigue, Frederic, Lawler, Jack, Glass, Christopher K, Awad, Issam A, and Ginsberg, Mark H

Subjects
Rare Diseases, Brain Disorders, Neurosciences, Good Health and Well Being, Animals, Cells, Cultured, Endothelial Cells, Gene Expression Profiling, Genetic Therapy, HEK293 Cells, Hemangioma, Cavernous, Central Nervous System, Humans, KRIT1 Protein, Kruppel-Like Factor 4, Kruppel-Like Transcription Factors, Mice, Inbred C57BL, Mice, Knockout, Mice, Transgenic, RNA Interference, Thrombospondin 1, Medical and Health Sciences, Immunology
Abstract

KRIT1 mutations are the most common cause of cerebral cavernous malformation (CCM). Acute Krit1 gene inactivation in mouse brain microvascular endothelial cells (BMECs) changes expression of multiple genes involved in vascular development. These changes include suppression of Thbs1, which encodes thrombospondin1 (TSP1) and has been ascribed to KLF2- and KLF4-mediated repression of Thbs1 In vitro reconstitution of TSP1 with either full-length TSP1 or 3TSR, an anti-angiogenic TSP1 fragment, suppresses heightened vascular endothelial growth factor signaling and preserves BMEC tight junctions. Furthermore, administration of 3TSR prevents the development of lesions in a mouse model of CCM1 (Krit1ECKO ) as judged by histology and quantitative micro-computed tomography. Conversely, reduced TSP1 expression contributes to the pathogenesis of CCM, because inactivation of one or two copies of Thbs1 exacerbated CCM formation. Thus, loss of Krit1 function disables an angiogenic checkpoint to enable CCM formation. These results suggest that 3TSR, or other angiogenesis inhibitors, can be repurposed for TSP1 replacement therapy for CCMs.

Published
2017

31. Endothelial TLR4 and the microbiome drive cerebral cavernous malformations.

Author

Tang, Alan T, Choi, Jaesung P, Kotzin, Jonathan J, Yang, Yiqing, Hong, Courtney C, Hobson, Nicholas, Girard, Romuald, Zeineddine, Hussein A, Lightle, Rhonda, Moore, Thomas, Cao, Ying, Shenkar, Robert, Chen, Mei, Mericko, Patricia, Yang, Jisheng, Li, Li, Tanes, Ceylan, Kobuley, Dmytro, Võsa, Urmo, Whitehead, Kevin J, Li, Dean Y, Franke, Lude, Hart, Blaine, Schwaninger, Markus, Henao-Mejia, Jorge, Morrison, Leslie, Kim, Helen, Awad, Issam A, Zheng, Xiangjian, and Kahn, Mark L

Subjects
Endothelial Cells, Animals, Humans, Mice, Gram-Negative Bacteria, Hemangioma, Cavernous, Central Nervous System, Disease Susceptibility, Lipopolysaccharides, Anti-Bacterial Agents, Injections, Intravenous, Germ-Free Life, Signal Transduction, Female, Male, Toll-Like Receptor 4, Immunity, Innate, Gastrointestinal Microbiome, Lipopolysaccharide Receptors, Hemangioma, Cavernous, Central Nervous System, Immunity, Innate, Injections, Intravenous, General Science & Technology
Abstract

Cerebral cavernous malformations (CCMs) are a cause of stroke and seizure for which no effective medical therapies yet exist. CCMs arise from the loss of an adaptor complex that negatively regulates MEKK3-KLF2/4 signalling in brain endothelial cells, but upstream activators of this disease pathway have yet to be identified. Here we identify endothelial Toll-like receptor 4 (TLR4) and the gut microbiome as critical stimulants of CCM formation. Activation of TLR4 by Gram-negative bacteria or lipopolysaccharide accelerates CCM formation, and genetic or pharmacologic blockade of TLR4 signalling prevents CCM formation in mice. Polymorphisms that increase expression of the TLR4 gene or the gene encoding its co-receptor CD14 are associated with higher CCM lesion burden in humans. Germ-free mice are protected from CCM formation, and a single course of antibiotics permanently alters CCM susceptibility in mice. These studies identify unexpected roles for the microbiome and innate immune signalling in the pathogenesis of a cerebrovascular disease, as well as strategies for its treatment.

Published
2017

32. Synopsis of Guidelines for the Clinical Management of Cerebral Cavernous Malformations: Consensus Recommendations Based on Systematic Literature Review by the Angioma Alliance Scientific Advisory Board Clinical Experts Panel

Author

Akers, Amy, Salman, Rustam Al-Shahi, Awad, Issam A, Dahlem, Kristen, Flemming, Kelly, Hart, Blaine, Kim, Helen, Jusue-Torres, Ignacio, Kondziolka, Douglas, Lee, Cornelia, Morrison, Leslie, Rigamonti, Daniele, Rebeiz, Tania, Tournier-Lasserve, Elisabeth, Waggoner, Darrel, and Whitehead, Kevin

Subjects
Biomedical and Clinical Sciences, Neurosciences, Clinical Sciences, Clinical Research, Brain Disorders, Advisory Committees, Central Nervous System Neoplasms, Consensus, Disease Management, Expert Testimony, Hemangioma, Cavernous, Hemangioma, Cavernous, Central Nervous System, Humans, Physical Therapy Modalities, Practice Guidelines as Topic, Stroke, United States, Cavernous, Angioma, Malformation, Guidelines, Recommendations, Neurology & Neurosurgery, Clinical sciences, Biological psychology
Abstract

BackgroundDespite many publications about cerebral cavernous malformations (CCMs), controversy remains regarding diagnostic and management strategies.ObjectiveTo develop guidelines for CCM management.MethodsThe Angioma Alliance ( www.angioma.org ), the patient support group in the United States advocating on behalf of patients and research in CCM, convened a multidisciplinary writing group comprising expert CCM clinicians to help summarize the existing literature related to the clinical care of CCM, focusing on 5 topics: (1) epidemiology and natural history, (2) genetic testing and counseling, (3) diagnostic criteria and radiology standards, (4) neurosurgical considerations, and (5) neurological considerations. The group reviewed literature, rated evidence, developed recommendations, and established consensus, controversies, and knowledge gaps according to a prespecified protocol.ResultsOf 1270 publications published between January 1, 1983 and September 31, 2014, we selected 98 based on methodological criteria, and identified 38 additional recent or relevant publications. Topic authors used these publications to summarize current knowledge and arrive at 23 consensus management recommendations, which we rated by class (size of effect) and level (estimate of certainty) according to the American Heart Association/American Stroke Association criteria. No recommendation was level A (because of the absence of randomized controlled trials), 11 (48%) were level B, and 12 (52%) were level C. Recommendations were class I in 8 (35%), class II in 10 (43%), and class III in 5 (22%).ConclusionCurrent evidence supports recommendations for the management of CCM, but their generally low levels and classes mandate further research to better inform clinical practice and update these recommendations. The complete recommendations document, including the criteria for selecting reference citations, a more detailed justification of the respective recommendations, and a summary of controversies and knowledge gaps, was similarly peer reviewed and is available on line www.angioma.org/CCMGuidelines .

Published
2017

36. Contributors

Author

Adams, Harold P., primary, Adeoye, Opeolu, additional, Albers, Gregory W., additional, Alexandrov, Andrei V., additional, Amin-Hanjani, Sepideh, additional, An, Hongyu, additional, Anderson, Craig S., additional, Anrather, Josef, additional, Aparicio, Hugo J., additional, Arai, Ken, additional, Aronowski, Jaroslaw, additional, Atchaneeyasakul, Kunakorn, additional, Audebert, Heinrich, additional, Auer, Roland N., additional, Awad, Issam A., additional, Ay, Hakan, additional, Baltan, Selva, additional, Balu, Ramani, additional, Behbahani, Mandana, additional, Benavente, Oscar R., additional, Bershad, Eric M., additional, Berthaud, Jimmy V., additional, Blackburn, Spiros L., additional, Bonati, Leo H., additional, Bösel, Julian, additional, Bousser, Marie Germaine, additional, Broderick, Joseph P., additional, Brown, Martin M., additional, Brown, Wendy, additional, Brust, John C.M., additional, Bushnell, Cheryl, additional, Canhão, Patrícia, additional, Caplan, Louis R., additional, Carrión-Penagos, Julián, additional, Castellanos, Mar, additional, Caunca, Michelle R., additional, Chabriat, Hugues, additional, Chamorro, Angel, additional, Chen, Jieli, additional, Chen, Jun, additional, Chopp, Michael, additional, Christorforids, Greg, additional, Connolly, E. Sander, additional, Cramer, Steven C., additional, Cucchiara, Brett L., additional, Czap, Alexandra L., additional, Dannenbaum, Mark J., additional, Davis, Patricia H., additional, Dawson, Ted M., additional, Dawson, Valina L., additional, Day, Arthur L., additional, De Silva, T. Michael, additional, de Sousa, Diana Aguiar, additional, Del Brutto, Victor J., additional, del Zoppo, Gregory J., additional, Derdeyn, Colin P., additional, Di Tullio, Marco R., additional, Diener, Hans Christoph, additional, Diringer, Michael N., additional, Dobkin, Bruce H., additional, Dzialowski, Imanuel, additional, Elkind, Mitchell S.V., additional, Elm, Jordan, additional, Feigin, Valery L., additional, Ferro, José Manuel, additional, Field, Thalia S., additional, Fischer, Marlene, additional, Fornage, Myriam, additional, Furie, Karen L., additional, Garcia-Bonilla, Lidia, additional, Giannotta, Steven L., additional, Gobin, Y. Pierre, additional, Goldberg, Mark P., additional, Goldstein, Larry B., additional, Gonzales, Nicole R., additional, Greer, David M., additional, Grotta, James C., additional, Guo, Ruiming, additional, Gutierrez, Jose, additional, Harmel, Peter, additional, Howard, George, additional, Howard, Virginia J., additional, Hwang, Jee-Yeon, additional, Iadecola, Costantino, additional, Jahan, Reza, additional, Jickling, Glen C., additional, Joutel, Anne, additional, Kasner, Scott E., additional, Katan, Mira, additional, Kellner, Christopher P., additional, Khan, Muhib, additional, Kidwell, Chelsea S., additional, Kim, Helen, additional, Kim, Jong S., additional, Kircher, Charles E., additional, Krings, Timo, additional, Krishnamurthi, Rita V., additional, Kurth, Tobias, additional, Lansberg, Maarten G., additional, Levy, Elad I., additional, Liebeskind, David S., additional, Liew, Sook-Lei, additional, Lin, David J., additional, Lisle, Benjamin, additional, Lo, Eng H., additional, Lyden, Patrick D., additional, Maki, Takakuni, additional, Maragkos, Georgios A., additional, Marosfoi, Miklos, additional, McCullough, Louise D., additional, Meckler, Jason M., additional, Meschia, James Frederick, additional, Messé, Steven R., additional, Mocco, J, additional, Mokin, Maxim, additional, Mooney, Michael A., additional, Morgenstern, Lewis B., additional, Moskowitz, Michael A., additional, Mullen, Michael T., additional, Nägel, Steffen, additional, Nedergaard, Maiken, additional, Neira, Justin A., additional, Newman, Sarah, additional, Nicholson, Patrick J., additional, Norrving, Bo, additional, O’Donnell, Martin, additional, Ofengeim, Dimitry, additional, Ogata, Jun, additional, Ogilvy, Christopher S., additional, Orrù, Emanuele, additional, Ortega-Gutiérrez, Santiago, additional, Padrick, Matthew Maximillian, additional, Parsha, Kaushik, additional, Parsons, Mark, additional, Patel, Neil V., additional, Patel, Virendra I., additional, Pawlikowska, Ludmila, additional, Pérez, Adriana, additional, Perez-Pinzon, Miguel A., additional, Picard, John M., additional, Polster, Sean P., additional, Powers, William J., additional, Puetz, Volker, additional, Putaala, Jukka, additional, Rabinovich, Margarita, additional, Ransom, Bruce R., additional, Roa, Jorge A., additional, Rosenberg, Gary A., additional, Rossitto, Christina P., additional, Rundek, Tatjana, additional, Russin, Jonathan J., additional, Sacco, Ralph L., additional, Safouris, Apostolos, additional, Samaniego, Edgar A., additional, Sansing, Lauren H., additional, Satani, Nikunj, additional, Sattenberg, Ronald J., additional, Saver, Jeffrey L., additional, Savitz, Sean I., additional, Schmidt, Christian, additional, Seshadri, Sudha, additional, Sharma, Vijay K., additional, Sharp, Frank R., additional, Sheth, Kevin N., additional, Siddiqi, Omar K., additional, Singhal, Aneesh B., additional, Sobey, Christopher G., additional, Sommer, Clemens J., additional, Spetzler, Robert F., additional, Stapleton, Christopher J., additional, Strickland, Ben A., additional, Su, Hua, additional, Suarez, José I., additional, Takayama, Hiroo, additional, Tarsia, Joseph, additional, Tatlisumak, Turgut, additional, Thomas, Ajith J., additional, Thompson, John W., additional, Tsivgoulis, Georgios, additional, Tournier-Lasserve, Elizabeth, additional, Vidal, Gabriel, additional, Wakhloo, Ajay K., additional, Weksler, Babette B., additional, Willey, Joshua Z., additional, Wintermark, Max, additional, Wong, Lawrence K.S., additional, Xi, Guohua, additional, Xu, Jinchong, additional, Yaghi, Shadi, additional, Yamaguchi, Takenori, additional, Yang, Tuo, additional, Yasaka, Masahiro, additional, Zahuranec, Darin B., additional, Zhang, Feng, additional, Zhang, John H., additional, Zheng, Zhitong, additional, Zukin, R. Suzanne, additional, and Zweifler, Richard M., additional

Published
2022
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39. PIK3CA and CCM mutations fuel cavernomas through a cancer-like mechanism

Author

Ren, Aileen A., Snellings, Daniel A., Su, Yourong S., Hong, Courtney C., Castro, Marco, Tang, Alan T., Detter, Matthew R., Hobson, Nicholas, Girard, Romuald, Romanos, Sharbel, Lightle, Rhonda, Moore, Thomas, Shenkar, Robert, Benavides, Christian, Beaman, M. Makenzie, Müller-Fielitz, Helge, Chen, Mei, Mericko, Patricia, Yang, Jisheng, Sung, Derek C., Lawton, Michael T., Ruppert, J. Michael, Schwaninger, Markus, Körbelin, Jakob, Potente, Michael, Awad, Issam A., Marchuk, Douglas A., and Kahn, Mark L.

Published
2021
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41. Does stereotactic thrombolysis with alteplase for intracerebral haemorrhage alter intraventricular haematoma volume? A secondary analysis of the MISTIE-III trial.

Author

Sun, Philip, Badihian, Shervin, Avadhani, Radhika, Walborn, Nathan, Yarava, Anusha, Alimoradi, Donya, Awad, Issam, Hanley, Daniel, Murthy, Santosh, and Ziai, Wendy

Subjects
INTRACEREBRAL hematoma, INSTITUTIONAL review boards, TISSUE plasminogen activator, INTRAVENTRICULAR hemorrhage, MEDIAN (Mathematics), LEUCOCYTES
Published
2024
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43. Hemorrhage Expansion Rates Before and After Minimally Invasive Surgery for Intracerebral Hemorrhage: Post Hoc Analysis of MISTIE II/III

Author

Ziai, Wendy C., primary, Badihian, Shervin, additional, Ullman, Natalie, additional, Thompson, Carol B., additional, Hildreth, Meghan, additional, Piran, Pirouz, additional, Montano, Nataly, additional, Vespa, Paul, additional, Martin, Neil, additional, Zuccarello, Mario, additional, Mayo, Steven W., additional, Awad, Issam, additional, and Hanley, Daniel F., additional

Published
2024
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46. Abstract WP224: Association of Quality-of-Life Domains and Clinical Symptoms in Pediatric Cerebral Cavernous Malformation Patients

Author

Chawla, Shweta, primary, Ortiz Ambrosio, Mateo, additional, Huynh, Nhu, additional, Nelson, Jeffrey, additional, McCulloch, Charles, additional, Vassar, Rachel, additional, Smith, Edward, additional, Vadivelu, Sudhakar, additional, Akers, Amy, additional, Lee, Cornelia, additional, Zabramski, Joseph M, additional, Torbey, Michel T, additional, Morrison, Leslie, additional, Awad, Issam A, additional, and Kim, Helen, additional

Published
2024
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48. Abstract TP12: Changes in Plasma Metabolites Reflect Lesional Iron Content and Permeability Imaging as Monitoring Biomarkers of Hemorrhage in Cavernous Angiomas

Author

Hage, Stephanie, primary, Bi, Dehua, additional, Vera cruz, Diana, additional, Xie, Bingqing, additional, Kinkade, Serena, additional, Little, Jessica, additional, Sidebottom, Ashley, additional, Alcazar-Felix, Roberto, additional, Lee, Juhyon, additional, Stadnik, Agnieszka, additional, Shenkar, Robert, additional, Carroll, Timothy, additional, Girard, Romuald, additional, Ji, Yuan, additional, and Awad, Issam A, additional

Published
2024
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