At Risk For Huntington Disease - The Pharos (Prospective Huntington At Risk Observational Study) Cohort Enrolled

Ira Shoulson,Karl Kieburtz,David Oakes,Elise Kayson,Hongwei Zhao, M. Aileen Shinaman, Megan Romer,Anne Young,Steven Hersch, Jack Penney,Kevin Biglan,Karen Marder,Jane Paulsen,Kimberly Quaid,Eric Siemers,Caroline Tanner, William Mallonee, David Palmer, Greg Suter,Richard Dubinsky, Gary Gronseth, R. Neil Schimke,Carolyn Gray,Martha Nance, Scott Bundlie, Dawn Radtke,Sandra Kostyk, George W. Paulson, Karen Thomas, Nonna Stepanov, Corrine Baic, James Caress,Francis Walker, Vicki Hunt,Sylvain Chouinard, Guy Rouleau, Hubert Poiffaut, Brigitte Rioux,Claudia Testa,Timothy Greenamyre, Joan Harrison,Jody Corey-Bloom,David Song,Guerry Peavy,Jody Goldstein,Jane Paulsen,Henry Paulson, Robert L. Rodnitzky,Ania Mikos, Becky Reese, Laura Stierman, Katie Williams, Lynn Vining,Karen Marder,Carol Moskowitz,Kimberly Quaid,Joanne Wojcieszek, Melissa Wesson,Ali Samii,Thomas Bird, Hillary Lipe,Norman Reynolds,Karen Blindauer, Jeannine Petit,Peter Como,Frederick Marshall, Timothy Counihan,Kevin Biglan,Carol Zimmerman,Penelope Hogarth, John Nutt, Pamela Andrews,Steven Hersch, Leslie Shinobu,Diana Rosas, Yoshio Kaneko, Sona Gevorkian, Paula Sexton,John Caviness,Charles Adler,Vicki Wheelock, David Richman, Teresa Tempkin, Chuang-Kuo Wu, Hubert Fernandez,Joseph H. Friedman, Margaret Lannon,Lauren Seeberger, Christopher O'Brien, Sherrie Montellano, Ninith Kartha, Sharin Sakurai, Susan Hickenbottom, Roger Albin, Kristine Wernette,Brad Racette,Joel S. Perlmutter, Laura Good, George Jackson,Susan Perlman, Shelley Segal, Russell Carroll, Laurie Carr,Wayne Martin, Ted Roberts,Marguerite Wieler,Blair Leavitt, Lorne Clarke,Lynn Raymond,Joji Decolongon, Vesna Popovska, Elisabeth Almqvist, William Ondo, Madhavi Thomas, Tetsuo Ashizawa,Joseph Jankovic, Robert Hauser,Juan Sanchez-Ramos, Karen Price, Holly Delgado, Sarah Furtado, Anne Louise Lafontaine,Oksana Suchowersky,Mary Lou Klimek, Rustom Sethna,Mark Guttman, Sandra Russell, Sheryl Elliott,Marc Mentis,Andrew Feigin,Marie Cox,Barbara Shannon,Alan Percy, Leon Dure, Donna Pendley, Jane Lane, Madaline Harrison, Elke Rost-Ruffner,William Johnson,Amy Colcher,Andrew Siderowf, Mary Matthews,Danna Jennings, Kenneth Marek, Karen Caplan,Stewart Factor, Donald Higgins,Eric Molho, Constance Nickerson,Sharon Evans, Douglas Hobson, Paul Shelton, Shaun Hobson,Carlos Singer,Nestor Galvez-Jimenez, William Koller, Doris Martin,Kelly Lyons, Dinorah Rodriguez, Kathleen Shannon,Cynthia Comella, Jean Jaglin, Karen Anderson,William Weiner, Kelly Dustin,Adam Rosenblatt, Christopher Ross, Deborah Pollard, Marie H. Saint-Hilaire, Peter Novak, J. Stephen Fink, Bonnie Hersh, Melissa Diggin, Leslie Vickers, Wallace Deckel, Mary Jane Fitzpatrick

Archives of neurology(2006)

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摘要
Objective: To identify the emerging clinical precursors that indicate the early onset of Huntington disease (HD) in a reliable and gene-specific manner. This information is critical for the development of therapeutic trials aimed at postponing clinical onset in HD gene carriers.Methods: Between July 1999 and January 2004, 1001 adults at 50-50 risk for HD agreed to provide longitudinal clinical data and a blood DNA sample under consent provisions that require their individual clinical and genetic information to never be revealed.Results: The Prospective Huntington At Risk Observational Study (PHAROS) cohort is characterized by a 2:1 predominance of women to men, high educational attainment, and gainful employment. Despite the gender disparity, the demographic, hereditary, and clinical characteristics of the female and male participants were similar. Investigators, who are unaware of individual gene status, characterized the baseline cohort to be highly functional with minimal motor or cognitive impairment; 92.3% of participants were judged to have no or nonspecific motor abnormalities; 6.7%, to have possible or probable motor signs; and only 1.0%, to have unequivocal HD.Conclusion: The baseline characteristics of the PHAROS cohort make it well suited to generate objective and prospective data about gene-specific clinical precursors that can be used as outcomes in controlled trials aimed at postponing the onset of HD.
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