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Pediatric neurology. 2013:49(6):439-44.DOI: 10.1016/j.pediatrneurol.2013.08.017

Subependymal giant cell astrocytoma: diagnosis, screening, and treatment. Recommendations from the international tuberous sclerosis complex consensus conference 2012

Roth, Jonathan; Roach, E Steve; Bartels, Ute; Jozwiak, Sergiusz; Koenig, Mary Kay; Weiner, Howard L; Franz, David N; Wang, Henry Z
BACKGROUND: Tuberous sclerosis complex is an autosomal dominant disorder predisposing to the development of benign lesions in different body organs, mainly in the brain, kidney, liver, skin, heart, and lung. Subependymal giant cell astrocytomas are characteristic brain tumors that occur in 10% to 20% of tuberous sclerosis complex patients and are almost exclusively related to tuberous sclerosis complex. Subependymal giant cell astrocytomas usually grow slowly, but their progression ultimately leads to the occlusion of the foramen of Monro, with subsequent increased intracranial pressure and hydrocephalus, thus necessitating intervention. During recent years, secondary to improved understanding in the biological and genetic basis of tuberous sclerosis complex, mammalian target of rapamycin inhibitors have been shown to be effective in the treatment of subependymal giant cell astrocytomas, becoming an alternative therapeutic option to surgery. METHODS: In June 2012, an International Tuberous Sclerosis Complex Consensus Conference was convened, during which an expert panel revised the diagnostic criteria and considered treatment options for subependymal giant cell astrocytomas. This article summarizes the subpanel's recommendations regarding subependymal giant cell astrocytomas. CONCLUSIONS: Mammalian target of rapamycin inhibitors have been shown to be an effective treatment of various aspects of tuberous sclerosis complex, including subependymal giant cell astrocytomas. Both mammalian target of rapamycin inhibitors and surgery have a role in the treatment of subependymal giant cell astrocytomas. Various subependymal giant cell astrocytoma-related conditions favor a certain treatment.
PMID: 24138953
ISSN: 0887-8994
CID: 669112
Journal of neurosurgery: Pediatrics. 2013:12(1):71-6.DOI: 10.3171/2013.4.PEDS12468

Longitudinal quantitative analysis of the tuber-to-brain proportion in patients with tuberous sclerosis

Hersh, David S; Chun, Jonathan; Weiner, Howard L; Pulitzer, Steven; Rusinek, Henry; Roth, Jonathan; Devinsky, Orrin; Milla, Sarah S
Object In patients with tuberous sclerosis complex (TSC), the tuber-to-brain proportion (TBP) is a marker of seizure severity and cognitive function. However, few studies have quantified the TBP. Furthermore, authors of these studies have measured the TBP at only a single time point, despite the fact that tuber cells were found to express proliferation markers, suggesting that they may be dynamic lesions. Authors of the present study used a semi-automated tuber segmentation program to determine whether the TBP changes over time. Methods Axial FLAIR MR images were retrospectively identified for patients with TSC who had undergone imaging at the authors' institution between February 1998 and June 2009. Using FireVoxel software, the TBP was measured for each patient at a minimum interval of 2 years. Results Twelve patients meeting the study inclusion criteria were identified. The mean TBP was 1.88% (range 0.38%-3.70%). Eight patients demonstrated minimal changes and 3 patients demonstrated small increases in TBP. The remaining patient exhibited a decrease of 1.00%, which correlated with a visible decrease in the size of 2 cerebellar lesions. Conclusions Semi-automated brain segmentation is a valuable tool in the longitudinal study of tubers. A subset of patients with TSC, particularly those with cerebellar lesions, may exhibit changes in the TBP over time.
PMID: 23662930
ISSN: 1933-0707
CID: 464182
Epilepsy & behavior. 2013:27(2):319-25.DOI: 10.1016/j.yebeh.2013.02.018

Brain MR spectroscopic abnormalities in "MRI-negative" tuberous sclerosis complex patients

Wu, William E; Kirov, Ivan I; Tal, Assaf; Babb, James S; Milla, Sarah; Oved, Joseph; Weiner, Howard L; Devinsky, Orrin; Gonen, Oded
Since approximately 5-10% of the ~50,000 tuberous sclerosis complex (TSC) patients in the US are "MRI-negative," our goal was to test the hypothesis that they nevertheless exhibit metabolic abnormalities. To test this, we used proton MR spectroscopy to obtain and compare gray and white matter (GM and WM) levels of the neuronal marker, N-acetylaspartate (NAA), the glial marker, myo-inositol (mI), and its associated creatine (Cr), and choline (Cho) between two "MRI-negative" female TSC patients (ages 5 and 43 years) and their matched controls. The NAA, Cr, Cho and mI concentrations, 9.8, 6.3, 1.4, and 5.7mM, in the pediatric control were similar to those of the patients, whereas the adult patient revealed a 17% WM NAA decrease and 16% WM Cho increase from their published means for healthy adults - both outside their respective 90% prediction intervals. These findings suggest that longer disease duration and/or TSC2 gene mutation may cause axonal dysfunction and demyelination.
PMCID:3644963
PMID: 23524469
ISSN: 1525-5050
CID: 301262
Epilepsy currents. 2013:13:347-347.DOI:

Evidence of increased neuroinflammation in human tuberous sclerosis complex potential implications for neurological dysfunction [Meeting Abstract]

Dilsiz, P; Ruppe, V; Weiner, H; Shoshkes, Reiss C; Najjar, S; French, J; Devinsky, O; Talos, D M
Rationale: Tuberous Sclerosis Complex (TSC) is a multisystem autosomal dominant disease caused by inactivating mutations in TSC1 or TSC2 genes. The most common neurological symptoms in TSC include treatment-resistant epilepsy, mental retardation and autism. There is now accumulating evidence that pro-inflammatory cytokines, produced and released mainly by reactive astrocytes and activated microglia, are implicated in a wide range of chronic neurological disorders, including refractory epilepsy. The purpose of this study was to evaluate the degree of inflammation in TSC brain lesions in human, with the hypothesis that activated glial cells and pro-inflammatory cytokines will be increased in both cortical tubers and peri-tuberal brain (PTB), possibly contributing to widespread network dysfunction. Methods: Human TSC specimens (n=10; ages 0-7 years) were prospectively collected following epilepsy surgery at NYULMC. Region-matched control autopsy brain samples from cases with normal neurological history were obtained from the Maryland Brain and Tissue Bank (n=7; ages 0-8 years). Tissue samples were collected and handled in accordance with the NYULMC Institutional Review Board. Fresh frozen specimens were used to prepare protein extracts for Western blotting. Blots were probed with the astrocytic and microglial markers GFAP and Iba1, as well as with the proinflammatory cytokines interleukin 1beta (IL-1beta) and tumor necrosis factor alpha (TNF-alpha). To determine statistical significance (p<0.05), oneway ANOVA followed by Student's t-test were used. Results: GFAP and Iba1 levels were significantly elevated in both tubers (343+/-115% of control, n=5; p<0.05 for GFAP, and 346+/-35% of control, n=5; p<0.0001 for Iba1) and PTB (225+/-37% of control, n=5; p<0.001 for GFAP, and 247+/-37% of control, n=5; p<0.001 for Iba1). The inactive pro-IL-1beta was highly upregulated in tubers (319+/-114% of control, n=6; p<0.05) and in PTB (228+/-70% of control, n=4; p<0.001), and this was accompanied by a commensur!
EMBASE:71196977
ISSN: 1535-7597
CID: 612732
AJNR. American journal of neuroradiology. 2013:34(3):655-9.DOI: 10.3174/ajnr.A3260

MRI Characterization and Longitudinal Study of Focal Cerebellar Lesions in a Young Tuberous Sclerosis Cohort

Vaughn, J; Hagiwara, M; Katz, J; Roth, J; Devinsky, O; Weiner, H; Milla, S
BACKGROUND AND PURPOSE:There are few articles characterizing cerebellar lesions in patients with TSC and no published series documenting longitudinal evaluation of these lesions, to our knowledge. Recent suggestion of a correlation between autism and cerebellar lesions in patients with TSC heightens the importance of understanding these lesions. Our purpose was to characterize cerebellar lesions in a cohort of young patients with TSC with specific interest in assessing longitudinal changes.MATERIALS AND METHODS:We retrospectively reviewed MR images from 145 pediatric and young adult patients with tuberous sclerosis (mean age, 7.6 years). A number of imaging characteristics of cerebellar tubers were recorded, and patients were evaluated for SGAs. Patients with follow-up scans >3 months from the original scan were further analyzed for longitudinal tuber characterization.RESULTS:There were 24.1% of patients with focal cerebellar lesions; 52.4% of patients with cerebellar lesions demonstrated change in imaging characteristics during longitudinal analysis. Fifty-one percent of the lesions were enhanced after gadolinium administration. Twenty percent of the patients with cerebellar lesions had pathologically confirmed SGAs compared with the incidence of 11% in the 145 patients with TSC reviewed.CONCLUSIONS:In our large cohort of young patients with TSC, cerebellar tubers were common and 52% of patients had tubers that changed with time. A higher percentage of patients with cerebellar lesions developed SGAs than patients with TSC without cerebellar lesions. Because this is the first reported longitudinal study of cerebellar lesions in TSC, further investigation may provide additional insight into TSC pathology and associated clinical manifestations, such as autism, developmental delay, and seizures.
PMID: 22954744
ISSN: 0195-6108
CID: 214232
Journal of neurosurgery: Pediatrics. 2013:11(3):268-73.DOI: 10.3171/2012.12.PEDS12338

The ability of high field strength 7-T magnetic resonance imaging to reveal previously uncharacterized brain lesions in patients with tuberous sclerosis complex

Chalifoux, Jason R; Perry, Nissa; Katz, Joel S; Wiggins, Graham C; Roth, Jonathan; Miles, Daniel; Devinsky, Orrin; Weiner, Howard L; Milla, Sarah S
Object Tuberous sclerosis complex (TSC) brain pathology is characterized on MRI by cortical tubers, subependymal nodules, and subependymal giant cell astrocytomas. Seizures, the prominent feature of TSC, are frequently intractable to medical therapy and, in many patients, resection of tubers results in seizure control. However, in approximately 40% of patients, resection of tubers does not control seizures. This fact, as well as evidence from invasive electrophysiological recordings and experimental animal models, suggests that in patients with TSC, there may be extratuberal epileptogenic brain that does not display any apparent abnormality on conventional MRI. The authors hypothesized that high field strength MRI might uncover lesions not seen on conventional MRI in these patients. Methods Institutional review board approval was obtained to scan 4 patients with TSC (ages 18-26 years) in a 7-T MR unit. Optimized 7-T sequences, including T1- and T2-weighted, FLAIR, SPACE FLAIR, T2*, and MPRAGE studies, were performed. Imaging studies were compared with identical sequences performed using a conventional 1.5-T MR scanner. Results In all 4 patients, there was improved visualization of the findings demonstrated on conventional imaging. Importantly, new lesions were detected in all 4 patients, which were not well visualized with conventional MRI. Newly detected lesions included microtubers, radial glial signal abnormalities, subependymal nodules arising from the caudate nucleus, and caudate nucleus lesions. Conclusions High field strength MRI detects previously uncharacterized lesions in patients with TSC and allows better detection and delineation of subtle abnormalities. In addition, the data demonstrate a compelling relationship between intraventricular lesions and the caudate nucleus. These data support previous electrophysiological and animal-model findings that demonstrate neurological pathology beyond the conventionally detected lesions in TSC.
PMID: 23289918
ISSN: 1933-0707
CID: 214222
Pediatric neurosurgery. 2013:49(2):99-104.DOI: 10.1159/000357357

Focal Resection of Leptomeningeal Angioma in a Rare Case of Sturge-Weber Syndrome without Facial Nevus

Shekhtman, Yevgenia; Kim, Irene; Riviello, James J Jr; Milla, Sarah S; Weiner, Howard L
Sturge-Weber syndrome (SWS) is a neurocutaneous disorder comprised typically of a facial nevus, leptomeningeal angioma with calcifications, and seizures. SWS without a port-wine stain is a rare variant with only 30 cases reported in the literature. Here, a case of an 8-year-old girl with no cutaneous abnormalities presenting with medically intractable epilepsy and MRI and CT findings consistent with SWS is described. The patient underwent multistage surgery with subdural electrode monitoring before and after resection of the epileptogenic focus, with complete excision of the lesion and postoperative resolution of her seizures. This is the first reported case of three-stage surgery for localized resection of the seizure focus for SWS. (c) 2014 S. Karger AG, Basel.
PMID: 24434861
ISSN: 1016-2291
CID: 882992
Lancet. 2012:380(9856):1829-39.DOI: 10.1016/S0140-6736(12)61768-1

Alemtuzumab for patients with relapsing multiple sclerosis after disease-modifying therapy: a randomised controlled phase 3 trial

Coles, Alasdair J; Twyman, Cary L; Arnold, Douglas L; Cohen, Jeffrey A; Confavreux, Christian; Fox, Edward J; Hartung, Hans-Peter; Havrdova, Eva; Selmaj, Krzysztof W; Weiner, Howard L; Miller, Tamara; Fisher, Elizabeth; Sandbrink, Rupert; Lake, Stephen L; Margolin, David H; Oyuela, Pedro; Panzara, Michael A; Compston, D Alastair S; Panitch, Hillel; Clifford, David; Antel, Jack; Barkhof, Frederik; Snydman, David; DeGroot, Leslie; Cines, Douglas; D'Agostino, Ralph; Greenberg, Benjamin; Krauss, Jörg; Limmroth, Volker; Markowitz, Clyde; Naismith, Robert; Tabby, David; Gupta, Ajay S; Fox, Edward; Glyman, Steven A; Thoits, Timothy K; Sullivan, Herman C; Cascione, Mark C; Rammohan, Kottil W; Gazda, Suzanne K; Wynn, Daniel R; Wray, Sibyl E; Elias, Stanton; Ford, Corey C; Goodman, Andrew; Hughes, Bruce L; Khan, Omar Azhar; Vaishnav, Anand G; Kirzinger, Stephen; Lynch, Sharon G; Mattson, David H; Braley, Tiffany J; Mikol, Daniel D; Krieger, Stephen; Miller, Aaron; Miller, Tamara Ann; Collins, Fort; Riskind, Peter N; Bomprezzi, Roberto; Wingerchuk, Dean M; Steingo, Brian; Cohen, Jeffrey Alan; Crayton, Heidi J; Royal, Walter 3rd; Twyman, Cary L; Cooper, Joanna A; Weiner, Leslie P; Moses, Harold Jr; Agius, Mark A; Bass, Ann Doan-Do; Lallana, Enrico C; Mitchell, Galen W; Krolczyk, Stanley J; Minagar, Alireza; Jubelt, Burk; Evans, Bradley K; Hunter, Samuel F; Rizvi, Syed A; Sheppard, Christopher A; Honeycutt, W M David; Herbert, Joseph; Lathi, Ellen S; Pardo, Gabriel; Ilenson, Lily Jung; Rothstein, Ted L; Thrower, Ben W; Picone, Mary Ann; Kita, Mariko; Grazioli, Erica M; Silliman, Scott L; Giancarlo, Thomas; Gottesman, Malcolm H; Zeid, Nuhad E Abou; Rowe, Vernon D 3rd; Boutwell, Christine M; Schaeffer, John D; LaGanke, Christopher C; Riley, Claire S; Gottschalk, Christopher; Preiningerova, Jana; Edwards, Keith R; Wendt, Jeanette K; Bigley, Kim Jr; Singer, Barry A; Shubin, Richard A; Markovic-Plese, Silva; Jones, Davis E; Clauser, Gary; Freedman, Mark S; Grand'Maison, Francois; Jacques, Francois H; Traboulsee, Anthony L; Brunet, Donald G; Kremenchutzky, Marcelo; Ayotte, Charles; Lava, Neil S; Waldman, Stephen R; Janus, Todd J; Vincent, Stephen Gerard; Gudesblatt, Mark; Rossen, Michael; Stein, Lee S; Machanic, Bennett-Irving; Vollmer, Timothy; Gitt, Jeffrey S; Dunn, Jeffrey; Negroski, Donald; Fletcher, Mark H; Javed, Adil; Frohman, Elliot M; Macdonell, Richard; Owen, John; Paine, Mark A; Boundy, Karyn; Broadley, Simon; Vucic, Steve; Reddel, Stephen; Dreyer, Michael D; Schwartz, Raymond; McCombe, Pamela Ann; Hodgkinson, Suzanne; Tilbery, Charles; Ferreira, Maria Lucia B; Callegaro, Dagoberto; Martins, Marcio Mena Barreto; Villanueva, Jesus Arturo Violante; Caballero, Noemi Santos; Mendoza, Claudia Venzor; Deri, Norma Haydee; Coles, Alasdair; Scolding, Neil James; Giovannoni, Gavin; Sharrack, Basil; Rog, David J; Comi, Giancarlo; Ghezzi, Angelo; Mancardi, Giovanni L; Durelli, Luca; Bertolotto, Antonio; Capra, Ruggero; Pozzilli, Carlo; Marrosu, Maria Giovanna; Hupperts, Raymond M M; van Munster, Erik; Montalbán, Xavier; González, Rafael Arroyo; Ayuso, Guillermo Izquierdo; Fernández, Óscar Fernández; Haya, Carlos; Confavreux, Christian; Vermersch, Patrick; de Seze, Jerome; Moreau, Thibault; Clavelou, Pierre; Lubetzki, Catherine; Clanet, Michel; Debouverie, Marc; Edan, Gilles; Hartung, Hans-Peter; Haas, Judith; Stangel, Martin; Ziemssen, Tjalf; Hemmer, Bernhard; Baum, Karl; Zettl, U Klaus; Herrlinger, U; Köhler, Wolfgang; Ochs, Gunter; Oschmann, Patrick; Tiel-Wilck, Klaus; Tumani, Hayrettin; Urban, Peter P; Lycke, Jan; Svenningsson, Anders; Kovarova, Ivana; Vachova, Marta; Rektor, Ivan; Talab, Radomir; Selmaj, Krzysztof; Stelmasiak, Zbigniew; Kozubski, Wojciech; Dubois, Benedicte D P; Dive, Dominique; Grandfossé, Rue; Sindic, Christian; Vass, Karl; Sørensen, Per Soelberg; Petersen, Thor; Ravnborg, Mads; Achiron, Anat; Dembinsky, Adi Vaknin; Karni, Arnon; Gusev, Evgeny I; Stolyarov, Igor D; Zavalishin, Igor A; Skoromets, Alexander A; Boyko, Alexei N; Belova, Anna N; Malkova, Nadezhda A; Barantsevich, Evgeniy R; Yakupov, Eduard Z; Perfiliev, Semen V; Poverennova, Irina E; Voloshyna, Natalia P; Nehrych, Tetyana I; Kobys, Tetyana O; Habek, Mario; Brinar, Vesna; Trkanjec, Zlatko; Vladić, Anton; Piskać, Spomenka Kidemet; Meštrovića, Ivana; Antonelli, Licia; Drulović, Jelena; Nadj, Čongor; Dinčić, Evica; Tončev, Gordana
BACKGROUND:The anti-CD52 monoclonal antibody alemtuzumab reduces disease activity in previously untreated patients with relapsing-remitting multiple sclerosis. We aimed to assess efficacy and safety of alemtuzumab compared with interferon beta 1a in patients who have relapsed despite first-line treatment. METHODS:In our 2 year, rater-masked, randomised controlled phase 3 trial, we enrolled adults aged 18-55 years with relapsing-remitting multiple sclerosis and at least one relapse on interferon beta or glatiramer. Eligible participants were randomly allocated in a 1:2:2 ratio by an interactive voice response system, stratified by site, to receive subcutaneous interferon beta 1a 44 μg, intravenous alemtuzumab 12 mg per day, or intravenous alemtuzumab 24 mg per day. Interferon beta 1a was given three-times per week and alemtuzumab was given once per day for 5 days at baseline and for 3 days at 12 months. The 24 mg per day group was discontinued to aid recruitment, but data are included for safety assessments. Coprimary endpoints were relapse rate and time to 6 month sustained accumulation of disability, comparing alemtuzumab 12 mg and interferon beta 1a in all patients who received at least one dose of study drug. This study is registered with ClinicalTrials.gov, number NCT00548405. FINDINGS/RESULTS:202 (87%) of 231 patients randomly allocated interferon beta 1a and 426 (98%) of 436 patients randomly allocated alemtuzumab 12 mg were included in the primary analyses. 104 (51%) patients in the interferon beta 1a group relapsed (201 events) compared with 147 (35%) patients in the alemtuzumab group (236 events; rate ratio 0·51 [95% CI 0·39-0·65]; p<0·0001), corresponding to a 49·4% improvement with alemtuzumab. 94 (47%) patients in the interferon beta 1a group were relapse-free at 2 years compared with 278 (65%) patients in the alemtuzumab group (p<0·0001). 40 (20%) patients in the interferon beta 1a group had sustained accumulation of disability compared with 54 (13%) in the alemtuzumab group (hazard ratio 0·58 [95% CI 0·38-0·87]; p=0·008), corresponding to a 42% improvement in the alemtuzumab group. For 435 patients allocated alemtuzumab 12 mg, 393 (90%) had infusion-associated reactions, 334 (77%) had infections (compared with 134 [66%] of 202 patients in the interferon beta 1a group) that were mostly mild-moderate with none fatal, 69 (16%) had thyroid disorders, and three (1%) had immune thrombocytopenia. INTERPRETATION/CONCLUSIONS:For patients with first-line treatment-refractory relapsing-remitting multiple sclerosis, alemtuzumab could be used to reduce relapse rates and sustained accumulation of disability. Suitable risk management strategies allow for early identification of alemtuzumab's main adverse effect of secondary autoimmunity. FUNDING/BACKGROUND:Genzyme (Sanofi) and Bayer Schering Pharma.
PMID: 23122650
ISSN: 1474-547x
CID: 5347992
Lancet. 2012:380(9856):1819-28.DOI: 10.1016/S0140-6736(12)61769-3

Alemtuzumab versus interferon beta 1a as first-line treatment for patients with relapsing-remitting multiple sclerosis: a randomised controlled phase 3 trial

Cohen, Jeffrey A; Coles, Alasdair J; Arnold, Douglas L; Confavreux, Christian; Fox, Edward J; Hartung, Hans-Peter; Havrdova, Eva; Selmaj, Krzysztof W; Weiner, Howard L; Fisher, Elizabeth; Brinar, Vesna V; Giovannoni, Gavin; Stojanovic, Miroslav; Ertik, Bella I; Lake, Stephen L; Margolin, David H; Panzara, Michael A; Compston, D Alastair S; Arnold, Doug; Panitch, Hillel; Clifford, David; Antel, Jack; Barkhof, Frederik; Snydman, David; DeGroot, Leslie; Cines, Douglas; D'Agostino, Ralph; Greenberg, Benjamin; Krauss, Jörg; Markowitz, Clyde; Naismith, Robert; Tabby, David; Gupta, Ajay S; Fox, Edward J; Glyman, Steven A; Cascione, Mark; Boster, Aaron; Rammohan, Kottil; Gazda, Suzanne; Wynn, Daniel R; Wray, Sibyl; Ford, Corey C; Goodman, Andrew; Hutton, George; Kaufman, Michael; Khan, Omar Azhar; Vaishnav, Anand; Kirzinger, Stephen; Lynch, Sharon G; Braley, Tiffany; Mikol, Daniel; Miller, Tamara; Ionete, Carolina; Riskind, Peter; Bomprezzi, Roberto; Carter, Jonathan; Steingo, Brian; Twyman, Cary; Bass, Ann; Lallana, Enrico; Kasper, Lloyd; Minagar, Alireza; Hunter, Samuel; Sheppard, Christopher; Herbert, Joseph; Pardo, Gabriel; Rowe, Vernon D; LaGanke, Christopher C; Edwards, Keith; Wendt, Jeanette K; Jones, David; Clauser, Gary; Vincent, Stephen Gerard; Gudesblatt, Mark; Freedman, Mark; Yeung, Michael; Grand'Maison, Francois; Jacques, Francois; Traboulsee, Anthony; Macdonell, Richard; King, John; Paine, Mark; Boundy, Karyn; Broadley, Simon; Vucic, Steve Ostoja; Reddel, Stephen; Dreyer, Michael; McCombe, Pamela; Ferreira, Maria Lucia; Callegaro, Dagoberto; Martins, Marcio Menna Barreto; Villanueva, Jesus Arturo Violante; Caballero, Noemi Santos; Deri, Norma Haydee; Coles, Alasdair; Robertson, Neil; Giovannoni, Gavin; Sharrack, Basil; Clanet, Michel; Haas, Judith; Stangel, Martin; Ziemssen, Tjalf; Baum, Karl; Faiss, Juergen; Ziemann, Ulf; Lycke, Jan; Kovarova, Ivana; Vachova, Marta; Selmaj, Krzysztof; Szczudlik, Andrzej; Stelmasiak, Zbigniew; Kozubski, Wojciech; Gusev, Evgeniy; Stolyarov, Igor; Zavalishin, Igor; Skoromets, Alexander; Boyko, Alexei; Belova, Anna; Malkova, Nadezhda; Barantsevich, Evgeniy; Yakupov, Eduard; Mishin, Gennadiy; Poverennova, Irina; Magzhanov, Rim; Orzheshkovskyi, Vasyl; Malyy, Volodymyr; Voloshyna, Natalia; Nehrych, Tetyana; Kobys, Tetyana; Habek, Mario; Brinar, Vesna; Trkanjec, Zlatko; Vladić, Anton; Antonelli, Licija; Rudež, Josip; Kidemet-Piskać, Spomenka; Drulović, Jelena; Nadj, Čongor; Dinčić, Evica; Vojinović, Slobodan; Stojanović, Miroslav; Pantović, Mihailo
BACKGROUND:The anti-CD52 monoclonal antibody alemtuzumab reduced disease activity in a phase 2 trial of previously untreated patients with relapsing-remitting multiple sclerosis. We aimed to assess efficacy and safety of first-line alemtuzumab compared with interferon beta 1a in a phase 3 trial. METHODS:In our 2 year, rater-masked, randomised controlled phase 3 trial, we enrolled adults aged 18-50 years with previously untreated relapsing-remitting multiple sclerosis. Eligible participants were randomly allocated in a 2:1 ratio by an interactive voice response system, stratified by site, to receive intravenous alemtuzumab 12 mg per day or subcutaneous interferon beta 1a 44 μg. Interferon beta 1a was given three-times per week and alemtuzumab was given once per day for 5 days at baseline and once per day for 3 days at 12 months. Coprimary endpoints were relapse rate and time to 6 month sustained accumulation of disability in all patients who received at least one dose of study drug. This study is registered with ClinicalTrials.gov, number NCT00530348. FINDINGS/RESULTS:187 (96%) of 195 patients randomly allocated interferon beta 1a and 376 (97%) of 386 patients randomly allocated alemtuzumab were included in the primary analyses. 75 (40%) patients in the interferon beta 1a group relapsed (122 events) compared with 82 (22%) patients in the alemtuzumab group (119 events; rate ratio 0·45 [95% CI 0·32-0·63]; p<0.0001), corresponding to a 54·9% improvement with alemtuzumab. Based on Kaplan-Meier estimates, 59% of patients in the interferon beta 1a group were relapse-free at 2 years compared with 78% of patients in the alemtuzumab group (p<0·0001). 20 (11%) of patients in the interferon beta 1a group had sustained accumulation of disability compared with 30 (8%) in the alemtuzumab group (hazard ratio 0·70 [95% CI 0·40-1·23]; p=0·22). 338 (90%) of patients in the alemtuzumab group had infusion-associated reactions; 12 (3%) of which were regarded as serious. Infections, predominantly of mild or moderate severity, occurred in 253 (67%) patients treated with alemtuzumab versus 85 (45%) patients treated with interferon beta 1a. 62 (16%) patients treated with alemtuzumab had herpes infections (predominantly cutaneous) compared with three (2%) patients treated with interferon beta 1a. By 24 months, 68 (18%) patients in the alemtuzumab group had thyroid-associated adverse events compared with 12 (6%) in the interferon beta 1a group, and three (1%) had immune thrombocytopenia compared with none in the interferon beta 1a group. Two patients in the alemtuzumab group developed thyroid papillary carcinoma. INTERPRETATION/CONCLUSIONS:Alemtuzumab's consistent safety profile and benefit in terms of reductions of relapse support its use for patients with previously untreated relapsing-remitting multiple sclerosis; however, benefit in terms of disability endpoints noted in previous trials was not observed here. FUNDING/BACKGROUND:Genzyme (Sanofi) and Bayer Schering Pharma.
PMID: 23122652
ISSN: 1474-547x
CID: 5347982
Journal of neurosurgery: Pediatrics. 2012:10(5):376-82.DOI: 10.3171/2012.8.PEDS1285

Electrocorticographic evidence of perituberal cortex epileptogenicity in tuberous sclerosis complex

Ma, Tracy S; Elliott, Robert E; Ruppe, Veronique; Devinsky, Orrin; Kuzniecky, Ruben; Weiner, Howard L; Carlson, Chad
Object Tuberous sclerosis complex (TSC) is a multisystem autosomal dominant disorder resulting in hamartomas of several organs. Cortical tubers are the most prominent brain lesions in TSC. Treatment-resistant epilepsy often develops early in life in patients with TSC and is associated with severe intellectual and behavioral impairments. Seizures may remit following epilepsy surgery in selected cases, yet it remains unclear whether the tuber or the perituberal cortex is the source of seizure onset. In this study, the authors reviewed the onset of seizures in patients in whom depth electrodes had been placed within or adjacent to cortical tubers. Methods After obtaining institutional review board approval, the authors retrospectively reviewed data from 12 pediatric patients with multifocal TSC and treatment-resistant epilepsy who had undergone invasive intracranial electroencephalographic monitoring. Tubers were identified on postimplantation MRI, and all depth electrodes were located. Depth electrode contacts were classified visually as either tuber/perituberal cortex or nontuber/nonperituberal cortex. Board-certified clinical neurophysiologists reviewed the seizures to identify all electrodes involved in the ictal onset. Results Among 309 recorded seizures, 104 unique ictal onset patterns were identified. Of the 11 patients with electrodes recording in a tuber, 9 had seizure onsets involving the tuber. Similarly, of the 9 patients with perituberal recording electrodes, 7 had perituberal ictal onsets. Overall, there was no difference in the percentage of contacts involved in seizure onset between the tuber and perituberal cortex. In a subset of 7 patients in whom at least 1 depth electrode contact was within the tuber and 1 was in the perituberal cortex, there was no difference between the percentage of tuber and perituberal onsets. Conclusions Findings demonstrated heterogeneity in the ictal onset patterns as well as involvement of the tuber and perituberal cortex within and between patients. Although the data are limited by the restricted region(s) sampled with intracranial electrodes, they do suggest that cortical hyperexcitability in TSC may derive from the tuber or surrounding cortex.
PMID: 22998031
ISSN: 1933-0707
CID: 183562