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Scientific reports. 2019:9(1).DOI: 10.1038/s41598-019-52894-z

Gut microbiome of treatment-naïve MS patients of different ethnicities early in disease course

Ventura, R E; Iizumi, T; Battaglia, T; Liu, Menghan; Perez-Perez, G I; Herbert, J; Blaser, M J
Although the intestinal microbiome has been increasingly implicated in autoimmune diseases, much is unknown about its roles in Multiple Sclerosis (MS). Our aim was to compare the microbiome between treatment-naïve MS subjects early in their disease course and controls, and between Caucasian (CA), Hispanic (HA), and African American (AA) MS subjects. From fecal samples, we performed 16S rRNA V4 sequencing and analysis from 45 MS subjects (15 CA, 16 HA, 14 AA) and 44 matched healthy controls, and whole metagenomic shotgun sequencing from 24 MS subjects (all newly diagnosed, treatment-naïve, and steroid-free) and 24 controls. In all three ethnic groups, there was an increased relative abundance of the same single genus, Clostridium, compared to ethnicity-matched controls. Analysis of microbiota networks showed significant changes in the network characteristics between combined MS cohorts and controls, suggesting global differences not restricted to individual taxa. Metagenomic analysis revealed significant enrichment of individual species within Clostridia as well as particular functional pathways in the MS subjects. The increased relative abundance of Clostridia in all three early MS cohorts compared to controls provides candidate taxa for further study as biomarkers or as etiologic agents in MS.
PMCID:6841666
PMID: 31705027
ISSN: 2045-2322
CID: 4186622
Lancet. 2018:391(10127):1263-1273.DOI: 10.1016/S0140-6736(18)30475-6

Siponimod versus placebo in secondary progressive multiple sclerosis (EXPAND): a double-blind, randomised, phase 3 study

Kappos, Ludwig; Bar-Or, Amit; Cree, Bruce A C; Fox, Robert J; Giovannoni, Gavin; Gold, Ralf; Vermersch, Patrick; Arnold, Douglas L; Arnould, Sophie; Scherz, Tatiana; Wolf, Christian; Wallström, Erik; Dahlke, Frank; Achiron, Anat; Achtnichts, Lutz; Agan, Kadriye; Akman-Demir, Gulsen; Allen, Alison B; Antel, Jack P; Antiguedad, Alfredo Rodriguez; Apperson, Michelle; Applebee, Angela M; Ayuso, Guillermo Izquierdo; Baba, Masayuki; Bajenaru, Ovidiu; Balasa, Rodica; Balci, Belgin Petek; Barnett, Michael; Bass, Ann; Becker, Veit U; Bejinariu, Mihaela; Bergh, Florian Then; Bergmann, Arnfin; Bernitsas, Evanthia; Berthele, Achim; Bhan, Virender; Bischof, Felix; Bjork, Randall John; Blevins, Gregg; Boehringer, Matthias; Boerner, Thomas; Bonek, Robert; Bowen, James D; Bowling, Allen; Boyko, Alexey N; Boz, Cavit; Bracknies, Vera; Braune, Stefan; Brescia Morra, Vincenzo; Brochet, Bruno; Brola, Waldemar; Brownstone, Paul Kenneth; Brozman, Miroslav; Brunet, Donald; Buraga, Ioan; Burnett, Margaret; Buttmann, Mathias; Butzkueven, Helmut; Cahill, Jonathan; Calkwood, Jonathan C; Camu, William; Cascione, Mark; Castelnovo, Giovani; Centonze, Diego; Cerqueira, Joao; Chan, Andrew; Cimprichova, Andrea; Cohan, Stanley; Comi, Giancarlo; Conway, Jill; Cooper, Joanna A; Corboy, John; Correale, Jorge; Costell, Brian; Cottrell, David A; Coyle, Patricia K; Craner, Matthew; Cui, Liying; Cunha, Luis; Czlonkowska, Anna; da Silva, Ana Martins; de Sa, Joao; de Seze, Jérôme; Debouverie, Marc; Debruyne, Jan; Decoo, Danny; Defer, Gilles; Derfuss, Tobias; Deri, Norma H; Dihenia, Bhupesh; Dioszeghy, Peter; Donath, Vladimir; Dubois, Benedicte; Duddy, Martin; Duquette, Pierre; Edan, Gilles; Efendi, Husnu; Elias, Stanton; Emrich, Peter J; Estruch, Bonaventura Casanova; Evdoshenko, Evgeniy P; Faiss, Juergen; Fedyanin, Alexander S; Feneberg, Wolfgang; Fermont, Jiske; Fernandez, Oscar Fernandez; Ferrer, Francisco Coret; Fink, Katharina; Ford, Helen; Ford, Corey; Francia, Ada; Freedman, Mark; Frishberg, Benjamin; Galgani, Simonetta; Garmany, George P; Gehring, Klaus; Gitt, Jeffrey; Gobbi, Claudio; Goldstick, Lawrence P; Gonzalez, Rafael Arroyo; Grandmaison, Francois; Grigoriadis, Nikolaos; Grigorova, Olga; Grimaldi, Luigi Maria Edoardo; Gross, Jeffrey; Gross-Paju, Katrin; Gudesblatt, Mark; Guillaume, Daniel; Haas, Judith; Hancinova, Viera; Hancu, Anca; Hardiman, Orla; Harmjanz, Arndt; Heidenreich, Fedor R; Hengstman, G J D; Herbert, Joseph; Herring, Mark; Hodgkinson, Suzanne; Hoffmann, Olaf M; Hofmann, Werner E; Honeycutt, William D; Hua, Le Hanh; Huang, Dehui; Huang, Yining; Huang, DeRen; Hupperts, Raymond; Imre, Piroska; Jacobs, Alan Keith; Jakab, Gabor; Jasinska, Elzbieta; Kaida, Kenichi; Kalnina, Jolanta; Kaprelyan, Ara; Karelis, Guntis; Karussis, Dimitrios; Katz, Amos; Khabirov, Farit A; Khatri, Bhupendra; Kimura, Takashi; Kister, Ilya; Kizlaitiene, Rasa; Klimova, Eleonora; Koehler, Juergen; Komatineni, Aparna; Kornhuber, Anselm; Kovacs, Krisztina; Koves, Agnes; Kozubski, Wojciech; Krastev, Georgi; Krupp, Lauren B; Kurca, Egon; Lassek, Christoph; Laureys, Guy; Lee, Liesly; Lensch, Eckart; Leutmezer, Fritz; Li, Hongzeng; Linker, Ralf A; Linnebank, Michael; Liskova, Petra; Llanera, Cristina; Lu, Jiahong; Lutterotti, Andreas; Lycke, Jan; Macdonell, Richard; Maciejowski, Maciej; Maeurer, Mathias; Magzhanov, Rim V; Maida, Eva-Maria; Malciene, Lina; Mao-Draayer, Yang; Marfia, Girolama Alessandra; Markowitz, Clyde; Mastorodimos, Vasileios; Matyas, Klotild; Meca-Lallana, Jose; Merino, Juan Antonio Garcia; Mihetiu, Ioan Gheorghe; Milanov, Ivan; Miller, Aaron E; Millers, Andrejs; Mirabella, Massimiliano; Mizuno, Masanori; Montalban, Xavier; Montoya, Lilina; Mori, Masahiro; Mueller, Stefanie; Nakahara, Jin; Nakatsuji, Yuji; Newsome, Scott; Nicholas, Richard; Nielsen, A Scott; Nikfekr, Esmaeil; Nocentini, Ugo; Nohara, Chiyoko; Nomura, Kyoichi; Odinak, Miroslav M; Olsson, Tomas; van Oosten, B W; Oreja-Guevara, Celia; Oschmann, Patrick; Overell, James; Pachner, Andrew; Panczel, Gyula; Pandolfo, Massimo; Papeix, Caroline; Patrucco, Liliana; Pelletier, Jean; Piedrabuena, Raul; Pless, Misha; Polzer, Udo; Pozsegovits, Krisztian; Rastenyte, Daiva; Rauer, Sebastian; Reifschneider, Gerd; Rey, Roberto; Rizvi, Syed A; Robertson, Derrick; Rodriguez, Jose Martinez; Rog, David; Roshanisefat, Homayoun; Rowe, Vernon; Rozsa, Csilla; Rubin, Susan; Rusek, Stanislaw; Saccà, Francesco; Saida, Takahiko; Salgado, Antonio Vasco; Sanchez, Victoria Eugenia Fernandez; Sanders, Kalina; Satori, Maria; Sazonov, Denis V; Scarpini, Elio Angelo; Schlegel, Eugen; Schluep, Myriam; Schmidt, Stephan; Scholz, Erich; Schrijver, H M; Schwab, Matthias; Schwartz, Raymond; Scott, James; Selmaj, Krzysztof; Shafer, Stuart; Sharrack, Basil; Shchukin, Ivan A; Shimizu, Yuko; Shotekov, Penko; Siever, Arno; Sigel, Karl-Otto; Silliman, Scott; Simo, Magdolna; Simu, Mihaela; Sinay, Vladimiro; Siquier, Antonio Escartin; Siva, Aksel; Skoda, Ondrej; Solomon, Andrew; Stangel, Martin; Stefoski, Dusan; Steingo, Brian; Stolyarov, Igor D; Stourac, Pavel; Strassburger-Krogias, Katrin; Strauss, Erik; Stuve, Olaf; Tarnev, Ivaylo; Tavernarakis, Antonios; Tello, Cristina Ramo; Terzi, Murat; Ticha, Veronika; Ticmeanu, Marina; Tiel-Wilck, Klaus; Toomsoo, Toomas; Tubridy, Niall; Tullman, Mark J; Tumani, Hayrettin; Turcani, Peter; Turner, Ben; Uccelli, Antonio; Urtaza, Francisco Javier Olascoaga; Vachova, Marta; Valikovics, Attila; Walter, Silke; Van Wijmeersch, Bart; Vanopdenbosch, Ludo; Weber, Joerg R; Weiss, Sara; Weissert, Robert; Vermersch, Patrick; West, Timothy; Wiendl, Heinz; Wiertlewski, Sandrine; Wildemann, Brigitte; Willekens, Barbara; Visser, L H; Vorobeychik, Galina; Xu, Xianhao; Yamamura, Takashi; Yang, Yi N; Yelamos, Sergio Martinez; Yeung, Michael; Zacharias, Alan; Zelkowitz, Marvin; Zettl, Uwe; Zhang, Meini; Zhou, Hongyu; Zieman, Ulf; Ziemssen, Tjalf
BACKGROUND:modulator, on disability progression in patients with SPMS. METHODS:This event-driven and exposure-driven, double-blind, phase 3 trial was done at 292 hospital clinics and specialised multiple sclerosis centres in 31 countries. Using interactive response technology to assign numbers linked to treatment arms, patients (age 18-60 years) with SPMS and an Expanded Disability Status Scale score of 3·0-6·5 were randomly assigned (2:1) to once daily oral siponimod 2 mg or placebo for up to 3 years or until the occurrence of a prespecified number of confirmed disability progression (CDP) events. The primary endpoint was time to 3-month CDP. Efficacy was assessed for the full analysis set (ie, all randomly assigned and treated patients); safety was assessed for the safety set. This trial is registered with ClinicalTrials.gov, number NCT01665144. FINDINGS:1651 patients were randomly assigned between Feb 5, 2013, and June 2, 2015 (1105 to the siponimod group, and 546 to the placebo group). One patient did not sign the consent form, and five patients did not receive study drug, all of whom were in the siponimod group. 1645 patients were included in the analyses (1099 in the siponimod group and 546 in the placebo). At baseline, the mean time since first multiple sclerosis symptoms was 16·8 years (SD 8·3), and the mean time since conversion to SPMS was 3·8 years (SD 3·5); 1055 (64%) patients had not relapsed in the previous 2 years, and 918 (56%) of 1651 needed walking assistance. 903 (82%) patients receiving siponimod and 424 (78%) patients receiving placebo completed the study. 288 (26%) of 1096 patients receiving siponimod and 173 (32%) of 545 patients receiving placebo had 3-month CDP (hazard ratio 0·79, 95% CI 0·65-0·95; relative risk reduction 21%; p=0·013). Adverse events occurred in 975 (89%) of 1099 patients receiving siponimod versus 445 (82%) of 546 patients receiving placebo; serious adverse events were reported for 197 (18%) patients in the siponimod group versus 83 (15%) patients in the placebo group. Lymphopenia, increased liver transaminase concentration, bradycardia and bradyarrhythmia at treatment initiation, macular oedema, hypertension, varicella zoster reactivation, and convulsions occurred more frequently with siponimod than with placebo. Initial dose titration mitigated cardiac first-dose effects. Frequencies of infections, malignancies, and fatalities did not differ between groups. INTERPRETATION:Siponimod reduced the risk of disability progression with a safety profile similar to that of other S1P modulators and is likely to be a useful treatment for SPMS. FUNDING:Novartis Pharma AG.
PMID: 29576505
ISSN: 1474-547x
CID: 5348122
Human brain mapping. 2017:38(8):4047-4063.DOI: 10.1002/hbm.23647

Proton MR spectroscopy of lesion evolution in multiple sclerosis: Steady-state metabolism and its relationship to conventional imaging

Kirov, Ivan I; Liu, Shu; Tal, Assaf; Wu, William E; Davitz, Matthew S; Babb, James S; Rusinek, Henry; Herbert, Joseph; Gonen, Oded
Although MRI assessment of white matter lesions is essential for the clinical management of multiple sclerosis, the processes leading to the formation of lesions and underlying their subsequent MRI appearance are incompletely understood. We used proton MR spectroscopy to study the evolution of N-acetyl-aspartate (NAA), creatine (Cr), choline (Cho), and myo-inositol (mI) in pre-lesional tissue, persistent and transient new lesions, as well as in chronic lesions, and related the results to quantitative MRI measures of T1-hypointensity and T2-volume. Within 10 patients with relapsing-remitting course, there were 180 regions-of-interest consisting of up to seven semi-annual follow-ups of normal-appearing white matter (NAWM, n = 10), pre-lesional tissue giving rise to acute lesions which resolved (n = 3) or persisted (n = 3), and of moderately (n = 9) and severely hypointense (n = 6) chronic lesions. Compared with NAWM, pre-lesional tissue had higher Cr and Cho, while compared with lesions, pre-lesional tissue had higher NAA. Resolving acute lesions showed similar NAA levels pre- and post-formation, suggesting no long-term axonal damage. In chronic lesions, there was an increase in mI, suggesting accumulating astrogliosis. Lesion volume was a better predictor of axonal health than T1-hypointensity, with lesions larger than 1.5 cm3 uniformly exhibiting very low (<4.5 millimolar) NAA concentrations. A positive correlation between longitudinal changes in Cho and in lesion volume in moderately hypointense lesions implied that lesion size is mediated by chronic inflammation. These and other results are integrated in a discussion on the steady-state metabolism of lesion evolution in multiple sclerosis, viewed in the context of conventional MRI measures. Hum Brain Mapp, 2017. (c) 2017 Wiley Periodicals, Inc.
PMCID:5510951
PMID: 28523763
ISSN: 1097-0193
CID: 2563072
Neurourology & urodynamics. 2017:36(4):1208-1213.DOI: 10.1002/nau.23101

Barriers experienced by patients with multiple sclerosis in seeking care for lower urinary tract symptoms

Brucker, Benjamin M; Nitti, Victor W; Kalra, Sidhartha; Herbert, Joseph; Sadiq, Areeba; Utomo, Puspa; Aponte, Margarita M
AIM: The Actionable Bladder Symptom and Screening Tool (ABSST) is used to identify multiple sclerosis (MS) patients in possible need of evaluation for urinary symptoms. The primary objective of this study was to identify barriers experienced by MS patients in seeking evaluation for urinary symptoms. We also assessed the utility of ABSST tool in identifying patients that will follow up with urologic evaluation. METHODS: This was a prospective observational study where 100 patients with MS were enrolled from an MS center. Patients completed demographic information, questions to assess barriers to care, a short form of the ABSST, and incontinence questionnaires. An ABSST score >3 met criteria for referral and evaluation. One year after enrollment, follow up calls assessed whether patients had seen a urinary specialist. RESULTS: The most common barriers to seeking care included "Doctor never referred" (16%) and "Doctor never asked" (13%). Thirty-eight percent (n = 8/21) of men stated "Doctor never referred" compared to 10% (n = 8/79) of women (P = 0.002). Twenty-seven patients had an ABSST Score >/=3 and were more interested in seeing a specialist compared to those scoring <3 (88.9%, n = 24/27 vs. 26%, n = 19/73; P = <0.001). After 1 year, 70 patients were reached for follow up. A total of 57.9% (n = 11/19) patients who followed up for evaluation screened positive on the ABSST. CONCLUSIONS: The ABSST is a valuable tool to identify MS patients with urinary symptoms who will likely follow up for genitourinary evaluation. However, other barriers beyond awareness exist and prevent patients from being evaluated.
PMID: 27548624
ISSN: 1520-6777
CID: 2221412
Neurology. 2016:87(19):1985-1992.DOI: 10.1212/WNL.0000000000003319

Alemtuzumab improves preexisting disability in active relapsing-remitting MS patients

Giovannoni, Gavin; Cohen, Jeffrey A; Coles, Alasdair J; Hartung, Hans-Peter; Havrdova, Eva; Selmaj, Krzysztof W; Margolin, David H; Lake, Stephen L; Kaup, Susan M; Panzara, Michael A; Compston, D Alastair S; Arnold, Doug; Confavreux, Christian; Fox, Edward; Weiner, Howard; 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; Deri, Norma Haydee; Boundy, Karyn; Broadley, Simon; Dreyer, Michael D; Hodgkinson, Suzanne; King, John Owen; Macdonell, Richard; Racp, Fafrm; McCombe, Pamela Ann; Paine, Mark A; Reddel, Stephen; Schwartz, Raymond; Vucic, Steve; Karl Vass, M D; Dominique Dive, PhD; Dubois, Benedicte D P; Sindic, Christian; Callegaro, Dagoberto; Ferreira, Maria Lucia B; Barreto Martins, Marcio Mena; Tilbery, Charles; Charles Ayotte; Brunet, Donald G; Freedman, Mark S; Grand'Maison, Francois; Jacques, Francois H; Kremenchutzky, Marcelo; Traboulsee, Anthony L; Licia Antonelli, M D; Brinar, Vesna; Habek, Mario; Piskać, Spomenka Kidemet; Trkanjec, Zlatko; Vladić, Anton; Ivana Kovarova; Rektor, Ivan; Talab, Radomir; Vachova, Marta; Petersen, Thor; Ravnborg, Mads; Sørensen, Per Soelberg; Michel Clanet; Clavelou, Pierre; de Seze, Jerome; Debouverie, Marc; Edan, Gilles; Lubetzki, Catherine; Moreau, Thibault; Vermersch, Patrick; Baum, Karl; Haas, Judith; Hemmer, Bernhard; Herrlinger, U; Köhler, Wolfgang; Ochs, Gunter; Stangel, Martin; Tumani, Hayrettin; Urban, Peter P; Zettl, U Klaus; Ziemssen, Tjalf; Anat Achiron; Karni, Arnon; Dembinsky, Adi Vaknin; Bertolotto, Antonio; Capra, Ruggero; Comi, Giancarlo; Durelli, Luca; Ghezzi, Angelo; Mancardi, Giovanni L; Marrosu, Maria Giovanna; Pozzilli, Carlo; Caballero, Noemi Santos; Mendoza, Claudia Venzor; Violante Villanueva, Jesus Arturo; Raymond M M Hupperts; van Munster, Erik; Wojciech Kozubski; Selmaj, Krzysztof; Stelmasiak, Zbigniew; Barantsevich, Evgeniy R; DMedSc; Belova, Anna N; Boyko, Alexei N; Gusev, Evgeny I; Malkova, Nadezhda A; Perfiliev, Semen V; Poverennova, Irina E; Skoromets, Alexander A; Stolyarov, Igor D; Yakupov, Eduard Z; Zavalishin, Igor A; Dinčić, Evica; Drulović, Jelena; Nadj, Čongor; Tončev, Gordana; González, Rafael Arroyo; Ayuso, Guillermo Izquierdo; Fernández, Óscar; Montalbán, Xavier; Jan Lycke; Svenningsson, Anders; Kobys, Tetyana O; Nehrych, Tetyana I; Voloshyna, Natalia P; Giovannoni, Gavin; Rog, David J; Scolding, Neil James; Sharrack, Basil; Abou Zeid, Nuhad E; Agius, Mark A; Doan-Do Bass, Ann; Bigley, G Kim Jr; Bomprezzi, Roberto; Boster, Aaron; Boutwell, Christine M; Braley, Tiffany J; Cascione, Mark C; Clauser, Gary; Cooper, Joanna A; Crayton, Heidi J; Dunn, Jeffrey; Edwards, Keith R; Elias, Stanton; Evans, Bradley K; Fletcher, Mark H; Ford, Corey C; Frohman, Elliot M; Gazda, Suzanne K; Giancarlo, Thomas; Gitt, Jeffrey S; Glyman, Steven A; Goodman, Andrew; Gottschalk, Christopher; Gottesman, Malcolm H; Grazioli, Erica M; Gudesblatt, Mark; Gupta, Ajay S; Herbert, Joseph; Honeycutt, W David; Hughes, Bruce L; Hunter, Samuel F; Janus, Todd J; Javed, Adil; Jones, Davis E; Jubelt, Burk; Henson, Lily Jung; Khan, Omar Azhar; Kita, Mariko; Kirzinger, Stephen; Krieger, Stephen; Krolczyk, Stanley J; LaGanke, Christopher C; Lallana, Enrico C; Lathi, Ellen S; Lava, Neil S; Lynch, Sharon G; Machanic, Bennett-Irving; Markovic-Plese, Silva; Mattson, David H; Mikol, Daniel D; Miller, Aaron; Miller, Tamara Ann; Minagar, Alireza; Mitchell, Galen W; Moses, Harold Jr; Negroski, Donald; Pardo, Gabriel; Picone, Mary Ann; Preiningerova, Jana; Rammohan, Kottil W; Riley, Claire S; Riskind, Peter N; Rizvi, Syed A; Rossen, Michael; Rothstein, Ted L; Rowe, Vernon D 3rd; Royal, Walter 3rd; Schaeffer, John D; Sheppard, Christopher A; Shubin, Richard A; Silliman, Scott L; Singer, Barry A; Stein, Lee S; Steingo, Brian; Sullivan, Herman C; Thoits, Timothy K; Thrower, Ben W; Twyman, Cary L; Vaishnav, Anand G; Vincent, Stephen Gerard; Vollmer, Timothy; Waldman, Stephen R; Weiner, Leslie P; Wendt, Jeanette K; Wingerchuk, Dean M; Wray, Sibyl E; Wynn, Daniel R
OBJECTIVE:To characterize effects of alemtuzumab treatment on measures of disability improvement in patients with relapsing-remitting multiple sclerosis (RRMS) with inadequate response (≥1 relapse) to prior therapy. METHODS:Comparison of Alemtuzumab and Rebif Efficacy in Multiple Sclerosis (CARE-MS) II, a 2-year randomized, rater-blinded, active-controlled, head-to-head, phase 3 trial, compared efficacy and safety of alemtuzumab 12 mg with subcutaneous interferon-β-1a (SC IFN-β-1a) 44 μg in patients with RRMS. Prespecified and post hoc disability outcomes based on Expanded Disability Status Scale (EDSS), Multiple Sclerosis Functional Composite (MSFC), and Sloan low-contrast letter acuity (SLCLA) are reported, focusing on improvement of preexisting disability in addition to slowing of disability accumulation. RESULTS:Alemtuzumab-treated patients were more likely than SC IFN-β-1a-treated patients to show improvement in EDSS scores (p < 0.0001) on all 7 functional systems. Significantly more alemtuzumab patients demonstrated 6-month confirmed disability improvement. The likelihood of improved vs stable/worsening MSFC scores was greater with alemtuzumab than SC IFN-β-1a (p = 0.0300); improvement in MSFC scores with alemtuzumab was primarily driven by the upper limb coordination and dexterity domain. Alemtuzumab-treated patients had more favorable changes from baseline in SLCLA (2.5% contrast) scores (p = 0.0014) and MSFC + SLCLA composite scores (p = 0.0097) than SC IFN-β-1a-treated patients. CONCLUSIONS:In patients with RRMS and inadequate response to prior disease-modifying therapies, alemtuzumab provides greater benefits than SC IFN-β-1a across several disability outcomes, reflecting improvement of preexisting disabilities. CLASSIFICATION OF EVIDENCE/METHODS:This study provides Class I evidence (based on rater blinding and a balance in baseline characteristics between arms) that alemtuzumab modifies disability measures favorably compared with SC IFN-β-1a.
PMCID:5109953
PMID: 27733571
ISSN: 1526-632x
CID: 5348132
Journal of neurology neurosurgery & psychiatry. 2016:87(8):885-9.DOI: 10.1136/jnnp-2015-312940

Extended interval dosing of natalizumab in multiple sclerosis

Zhovtis Ryerson, L; Frohman, T C; Foley, J; Kister, I; Weinstock-Guttman, B; Tornatore, C; Pandey, K; Donnelly, S; Pawate, S; Bomprezzi, R; Smith, D; Kolb, C; Qureshi, S; Okuda, D; Kalina, J; Rimler, Z; Green, R; Monson, N; Hoyt, T; Bradshaw, M; Fallon, J; Chamot, E; Bucello, M; Beh, S; Cutter, G; Major, E; Herbert, J; Frohman, E M
BACKGROUND: Natalizumab (NTZ), a monoclonal antibody to human alpha4beta1/beta7 integrin, is an effective therapy for multiple sclerosis (MS), albeit associated with progressive multifocal leukoencephalopathy (PML). Clinicians have been extending the dose of infusions with a hypothesis of reducing PML risk. The aim of the study is to evaluate the clinical consequences of reducing NTZ frequency of infusion up to 8 weeks 5 days. METHODS: A retrospective chart review in 9 MS centres was performed in order to identify patients treated with extended interval dosing (EID) regimens of NTZ. Patients were stratified into 3 groups based on EID NTZ treatment schedule in individual centres: early extended dosing (EED; n=249) every 4 weeks 3 days to 6 weeks 6 days; late extended dosing (LED; n=274) every 7 weeks to 8 weeks 5 days; variable extended dosing (n=382) alternating between EED and LED. These groups were compared with patients on standard interval dosing (SID; n=1093) every 4 weeks. RESULTS: 17% of patients on SID had new T2 lesions compared with 14% in EID (p=0.02); 7% of patients had enhancing T1 lesions in SID compared with 9% in EID (p=0.08); annualised relapse rate was 0.14 in the SID group, and 0.09 in the EID group. No evidence of clinical or radiographic disease activity was observed in 62% of SID and 61% of EID patients (p=0.83). No cases of PML were observed in EID group compared with 4 cases in SID cohort. CONCLUSIONS: Dosing intervals up to 8 weeks 5 days did not diminish effectiveness of NTZ therapy. Further monitoring is ongoing to evaluate if the risk of PML is reduced in patients on EID.
PMID: 26917698
ISSN: 1468-330x
CID: 1965552
BMC neurology. 2016:16.DOI: 10.1186/s12883-016-0623-2

Factors associated with benign multiple sclerosis in the New York State MS Consortium (NYSMSC)

Zivadinov, Robert; Cookfair, Diane L; Krupp, Lauren; Miller, Aaron E; Lava, Neil; Coyle, Patricia K; Goodman, Andrew D; Jubelt, Burk; Lenihan, Michael; Herbert, Joseph; Gottesman, Malcolm; Snyder, David H; Apatoff, Brian R; Teter, Barbara E; Perel, Allan B; Munschauer, Frederick; Weinstock-Guttman, Bianca
BACKGROUND: This retrospective analysis explored prognostic factors associated with a benign multiple sclerosis (BMS) disease course at baseline and over the 4-year follow-up. METHODS: Patients from the centralized New York State Multiple Sclerosis Consortium registry were classified as having BMS according to 3 different criteria centered on disease duration and disability. Additional analyses explored prognostic factors associated with BMS using the most conservative disability criteria (Expanded Disability Status Scale /=10 years). RESULTS: Among 6258 patients who fulfilled eligibility criteria, 19.8 % to 33.3 % were characterized as having BMS, at baseline depending on classification criteria used. Positive prognostic factors for BMS at baseline included female sex (p < 0.0001) and younger age at onset (p < 0.0001); negative prognostic factors included progressive-onset type of MS and African-American race. Of the 1237 BMS patients (per most conservative criteria), 742 were followed for a median of 4 years to explore effect of disease-modifying treatment (DMT) on benign status. DMT (p = 0.009) and longer disease duration (p = 0.007) were the only significant positive predictors of maintaining BMS at follow-up. The protective effect was stronger for patients taking DMT at both enrollment and follow-up (OR = 0.71; p = 0.006). CONCLUSIONS: There is a need for development of more reliable prognostic indicators of BMS. Use of DMT was significantly associated with maintaining a benign disease state.
PMCID:4946222
PMID: 27416843
ISSN: 1471-2377
CID: 2180222
Journal of neurology. 2016:263(6):1146-55.DOI: 10.1007/s00415-016-8118-z

Quantification of normal-appearing white matter tract integrity in multiple sclerosis: a diffusion kurtosis imaging study

de Kouchkovsky, Ivan; Fieremans, Els; Fleysher, Lazar; Herbert, Joseph; Grossman, Robert I; Inglese, Matilde
Our aim was to characterize the nature and extent of pathological changes in the normal-appearing white matter (NAWM) of patients with multiple sclerosis (MS) using novel diffusion kurtosis imaging-derived white matter tract integrity (WMTI) metrics and to investigate the association between these WMTI metrics and clinical parameters. Thirty-two patients with relapsing-remitting MS and 19 age- and gender-matched healthy controls underwent MRI and neurological examination. Maps of mean diffusivity, fractional anisotropy and WMTI metrics (intra-axonal diffusivity, axonal water fraction, tortuosity and axial and radial extra-axonal diffusivity) were created. Tract-based spatial statistics analysis was performed to assess for differences in the NAWM between patients and controls. A region of interest analysis of the corpus callosum was also performed to assess for group differences and to evaluate correlations between WMTI metrics and measures of disease severity. Mean diffusivity and radial extra-axonal diffusivity were significantly increased while fractional anisotropy, axonal water fraction, intra-axonal diffusivity and tortuosity were decreased in MS patients compared with controls (p values ranging from <0.001 to <0.05). Axonal water fraction in the corpus callosum was significantly associated with the expanded disability status scale score (rho = -0.39, p = 0.035). With the exception of the axial extra-axonal diffusivity, all metrics were correlated with the symbol digits modality test score (p values ranging from 0.001 to <0.05). WMTI metrics are thus sensitive to changes in the NAWM of MS patients and might provide a more pathologically specific, clinically meaningful and practical complement to standard diffusion tensor imaging-derived metrics.
PMCID:5369414
PMID: 27094571
ISSN: 1432-1459
CID: 2079962
Multiple sclerosis & related disorders. 2015:4(6):495-8.DOI: 10.1016/j.msard.2015.08.008

Natalizumab-induced hepatic injury: A case report and review of literature

Antezana, A; Sigal, S; Herbert, J; Kister, I
Natalizumab is an alpha4-integrin monoclonal antibody used for treatment of relapsing multiple sclerosis (MS). At least and nearly 30 cases of liver failure in natalizumab-treated patients are listed in the post-marketing FDA adverse event reporting system (FAERS) and twelve patients with severe liver injury, including several after the first infusion, have been reported (Lisotti et al., 2012; Bezabeh et al., 2010; Martinez-Lapiscina et al., 2013; Michael et al., 2007; Hillen et al., 2015). Herein, we describe a case of a young woman with relapsing MS who developed acute liver injury after the second infusion of natalizumab. Liver biopsy demonstrated a mixed pattern of medication-induced injury or partially treated auto-immune hepatitis. Liver function normalized after natalizumab discontinuation and a subsequent liver biopsy showed resolution of hepatitis. The patient's MS has since been successfully treated with rituximab for over a year. We review the published cases of liver injury associated with natalizumab and those in the post-marketing FDA adverse event reporting system (FAERS).
PMID: 26590653
ISSN: 2211-0356
CID: 1856282
Human brain mapping. 2015:36(10):3749-3760.DOI: 10.1002/hbm.22875

Effect of in-painting on cortical thickness measurements in multiple sclerosis: A large cohort study

Govindarajan, Koushik A; Datta, Sushmita; Hasan, Khader M; Choi, Sangbum; Rahbar, Mohammad H; Cofield, Stacey S; Cutter, Gary R; Lublin, Fred D; Wolinsky, Jerry S; Narayana, Ponnada A; Agius, M; Bashir, K; Baumhefner, R; Birnbaum, G; Blevins, G; Bomprezzi, R; Boster, A; Brown, T; Burkholder, J; Camac, A; Campagnolo, D; Carter, J; Cohen, B; Cooper, J; Corboy, J; Cross, A; Dewitt, L; Dunn, J; Edwards, K; Eggenberger, E; English, J; Felton, W; Fodor, P; Ford, C; Freedman, M; Galetta, S; Garmany, G; Goodman, A; Gottesman, M; Gottschalk, C; Gruental, M; Gudesblatt, M; Hamill, R; Herbert, J; Holub, R; Honeycutt, W; Hughes, B; Hutton, G; Jacobs, D; Johnson, K; Kasper, L; Kattah, J; Kaufman, M; Keegan, M; Khan, O; Khatri, B; Kita, M; Koffman, B; Lallana, E; Lava, N; Lindsey, J; Loge, P; Lynch, S; McGee, F; Mejico, L; Metz, L; O'Connor, P; Pandey, K; Panitch, H; Preiningerova, J; Rammohan, K; Riley, C; Riskind, P; Rolak, L; Royal, W; Scarberry, S; Schulman, A; Scott, T; Sheppard, C; Sheremata, W; Stone, L; Stuart, W; Subramaniam, S; Thadani, V; Thomas, F; Louis, Saint; Thrower, B; Tullman, M; Turel, A; Vollmer, T; Waldman, S; Weinstock-Guttman, B; Wendt, J; Williams, R; Wynn, D; Yeung, M
A comprehensive analysis of the effect of lesion in-painting on the estimation of cortical thickness using magnetic resonance imaging was performed on a large cohort of 918 relapsing-remitting multiple sclerosis patients who participated in a phase III multicenter clinical trial. An automatic lesion in-painting algorithm was developed and implemented. Cortical thickness was measured using the FreeSurfer pipeline with and without in-painting. The effect of in-painting was evaluated using FreeSurfer's paired analysis pipeline. Multivariate regression analysis was also performed with field strength and lesion load as additional factors. Overall, the estimated cortical thickness was different with in-painting than without. The effect of in-painting was observed to be region dependent, more significant in the left hemisphere compared to the right, was more prominent at 1.5 T relative to 3 T, and was greater at higher lesion volumes. Our results show that even for data acquired at 1.5 T in patients with high lesion load, the mean cortical thickness difference with and without in-painting is ∼2%. Based on these results, it appears that in-painting has only a small effect on the estimated regional and global cortical thickness. Hum Brain Mapp 36:3749-3760, 2015. © 2015 Wiley Periodicals, Inc.
PMCID:4839289
PMID: 26096844
ISSN: 1097-0193
CID: 5348142