Abstract
Leukocyte 8-hydroxydeoxyguanosine (8OHdG) is an indicator of oxidative stress, impaired metabolism, and mitochondrial dysfunction, features that have been implicated in Huntington disease (HD). Increased levels of 8OHdG have been reported in the caudate, parietal cortex, and peripherally in the serum and leukocytes, in patients diagnosed with HD. However, little is known about levels in prodromal patients and changes that might occur as the disease progresses. To address these issues, 8OHdG was tracked over time for a subset of participants enrolled in the PREDICT-HD study. Participants were stratified into four groups based on proximity to HD diagnosis at study entry: Controls (gene-negative individuals), Low (low probability of near-future diagnosis), Medium, and High. Blood samples were analyzed using Liquid Chromatography Electrochemical Array, and for comparison purposes, a separate cross-sectional sample was analyzed using liquid chromatography coupled with multiple-reaction-monitoring mass spectrometry. Longitudinal data analysis showed that initial status (at study entry) and annual rate of change varied as a function of proximity group, adjusting for sex, education, age at study entry, and site effects. Overall levels were lowest for the Control group and highest for the High group, and the rate of increase varied in a similar manner. The finding that 8OHdG concentrations increased as a function of proximity to projected disease diagnosis and duration indicates support for the continued assessment of 8OHdG as a robust clinical HD biomarker.
Original language | English |
---|---|
Pages (from-to) | 625-634 |
Number of pages | 10 |
Journal | Neurobiology of Disease |
Volume | 46 |
Issue number | 3 |
DOIs | |
Publication status | Published - Jun 2012 |
Keywords
- 8OHdG
- Biomarker
- Huntington disease
- Mitochondrial dysfunction
- Oxidative stress
- PREDICT-HD
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In: Neurobiology of Disease, Vol. 46, No. 3, 06.2012, p. 625-634.
Research output: Contribution to journal › Article › Research › peer-review
TY - JOUR
T1 - 8OHdG as a marker for Huntington disease progression
AU - Long, Jeffrey D.
AU - Matson, Wayne R.
AU - Juhl, Andrew
AU - Leavitt, Blair R.
AU - Paulsen, Jane S.
AU - Wassink, Thomas
AU - Cross, Stephen
AU - Doucette, Nicholas
AU - Kimble, Mycah
AU - Ryan, Patricia
AU - Wood, Jessica
AU - Epping, Eric A.
AU - Beglinger, Leigh
AU - Chiu, Edmond
AU - Yastrubetskaya, Olga
AU - Preston, Joy
AU - Goh, Anita
AU - Fonseka, Chathushka
AU - Ronsisvalle, Liz
AU - Chua, Phyllis
AU - Komiti, Angela
AU - Raymond, Lynn
AU - Santos, Rachelle Dar
AU - Decolongon, Joji
AU - Rosenblatt, Adam
AU - Ross, Christopher
AU - Shpritz, Barnett
AU - Welsh, Claire
AU - Mallonee, William M.
AU - Suter, Greg
AU - Addison, Judy
AU - Samii, Ali
AU - Macaraeg, Alma
AU - Jones, Randi
AU - Wood-Siverio, Cathy
AU - Factor, Stewart A.
AU - Testa, Claudia
AU - Barker, Roger A.
AU - Mason, Sarah
AU - Goodman, Anna
AU - Swain, Rachel
AU - Dipietro, Anna
AU - McCusker, Elizabeth
AU - Griffith, Jane
AU - Loy, Clement
AU - Gunn, David
AU - Stewart, Linda
AU - Landwehrmeyer, Bernhard G.
AU - Orth, Michael
AU - Süβmuth, Sigurd
AU - Barth, Katrin
AU - Trautmann, Sonja
AU - Quaid, Kimberly
AU - Wesson, Melissa
AU - Wojcieszek, Joanne
AU - Guttman, Mark
AU - Sheinberg, Alanna
AU - Karmalkar, Irita
AU - Perlman, Susan
AU - Johnson, Arik
AU - Geschwind, Michael D.
AU - Gooblar, Jon
AU - Kang, Gail
AU - Warner, Tom
AU - Burrows, Maggie
AU - Novak, Marianne
AU - Andrews, Thomasin
AU - Rosser, Elisabeth
AU - Tabrizi, Sarah
AU - Rosser, Anne
AU - Price, Kathy
AU - Hunt, Sarah
AU - Marshall, Frederick
AU - Chesire, Amy
AU - Wodarski, Mary
AU - Hickey, Charlyne
AU - Suchowersky, Oksana
AU - Furtado, Sarah
AU - Klimek, Mary Lou
AU - Panegyres, Peter
AU - Vuletich, Elizabeth
AU - Andrew, Steve
AU - Zombor, Rachel
AU - Perlmutter, Joel
AU - Barton, Stacey
AU - Schmidt, Amy
AU - Miedzybrodzka, Zosia
AU - Simpson, Sheila A.
AU - Rae, Daniela
AU - D'alessandro, Mariella
AU - Craufurd, David
AU - Fullam, Ruth
AU - Howard, Elizabeth
AU - Mazzoni, Pietro
AU - Marder, Karen
AU - Wasserman, Paula
AU - Kumar, Rajeev
AU - Erickson, Diane
AU - Wheelock, Vicki
AU - Tempkin, Terry
AU - Mans, Nicole
AU - Baynes, Kathleen
AU - Jankovic, Joseph
AU - Hunter, Christine
AU - Ondo, William
AU - de Yebenes, Justo Garcia
AU - Garde, Monica Bascunana
AU - Fatas, Marta
AU - Martinez-Descales, Asuncion
AU - Martin, Wayne
AU - King, Pamela
AU - Sran, Satwinder
AU - Ahmed, Anwar
AU - Rao, Stephen
AU - Reece, Christine
AU - Zimbelman, Janice
AU - Bea, Alexandra
AU - Newman, Emily
AU - Bura, Alex
AU - Johnson, Hans
AU - Smith, Megan M.
AU - Williams, Janet
AU - Beglinger, Leigh
AU - Mills, James
AU - Aylward, Elizabeth
AU - Biglan, Kevin
AU - Macdonald, Marcy
AU - Nance, Martha
AU - Erwin, Cheryl
AU - Hayden, Michael
AU - Didonato, Stefano
AU - Evans, Ken
AU - Peterson, Asa
AU - Borowsky, Beth
AU - Juhl, Andrew
AU - Weir, David
AU - Vonsattell, Jean Paul
AU - Moskowitz, Carol
AU - Leserman, Anne
AU - Schaul, Lynn
AU - Vik, Stacie
AU - Harrington, Deborah
AU - Castillo, Gabriel
AU - Morison, Jessica
AU - Reed, Jason
AU - Diaz, Michael
AU - Dobbins, Ian
AU - Hershey, Tamara
AU - Foster, Erin
AU - Moore, Deborah
AU - Westervelt, Holly
AU - Davis, Jennifer
AU - Tremont, Geoff
AU - Moser, David J.
AU - Rowe, Kelly
AU - Theriault, Danielle
AU - Gehl, Carissa
AU - Matheson, Kirsty
AU - Siedlecki, Karen
AU - Van Walsem, Marleen
AU - Bonner, Susan
AU - Elias, Greg
AU - Faust, Melanie
AU - Borowski, Beth
AU - Carlozzi, Noelle
AU - Duff, Kevin
AU - Georgiou-Karistianis, Nellie
AU - Stout, Julie
AU - Lange, Herwig
AU - Papp, Kate
AU - Ro, Eunyoe
AU - Clark, Lee Anna
AU - Downing, Nancy
AU - Laing, Joan
AU - Rees, Kristine
AU - Ready, Rebecca
AU - Vaccarino, Anthony
AU - Farias, Sarah
AU - Gusella, Jim
AU - Myers, Rick
AU - Juhl, Andrew
AU - Wang, Kai
AU - Ross, Christopher
AU - Pierson, Ron
AU - Jones, Kathy
AU - Marietta, Jacquie
AU - McDowell, William
AU - Harris, Greg
AU - Kim, Eun Young
AU - Ashburner, John
AU - Potkin, Steve
AU - Toga, Arthur
AU - Axelson, Eric
AU - Miller, Michael
AU - Reading, Sarah
AU - Beg, Mirza Faisal
AU - Magnotta, Vincent A.
AU - Helmer, Karl
AU - Lim, Kelvin
AU - Lowe, Mark
AU - Mori, Sasumu
AU - Song, Allen
AU - Turner, Jessica
AU - Beall, Erik
AU - Koenig, Katherine
AU - Phillips, Michael
AU - Bryant, April
AU - Corey-Bloom, Jody
AU - Reilmann, Ralf
AU - Unds, Zerka
AU - Fiedorowicz, Jess
AU - Robinson, Robert
AU - Ruggle, Adam
AU - Liu, Dawei
AU - Anderson, Karen
AU - Groves, Mark
AU - Rickards, Hugh
AU - van Duijn, Eric
AU - Antonijevic, Irina
AU - Giuliano, Joseph
AU - Lu, Wenjing
AU - Lourens, Spencer
AU - Zhang, Ying
AU - Kimble, Mycah
AU - Thumma, Kelli
AU - Waterman, Elijah
AU - Hinkel, Jeremy
AU - Schaul, Lynn
AU - Hughes, Lisa
AU - Connell, R. J.
AU - Pease, Karen
AU - Rogers, Ben
AU - Smith, Jim
AU - Wu, Shuhua
AU - Zschiegner, Roland
AU - Carney, Erin
AU - McKirgan, Bill
AU - Scully, Mark
AU - Wyse, Ryan
AU - Bockholt, Jeremy
AU - Werling-Witkoske, Chris
AU - Anderson, Karla
AU - Rapp, Jennifer
AU - Dudler, Ann
AU - Schumacher, Jamy
AU - Thompson, Sean
AU - Davis, Leann
AU - Henneberry, Machelle
AU - Ennis, Greg
AU - Blanchard, Steve
AU - the PREDICT-HD Investigators and Coordinators of the Huntington Study Group
N1 - Funding Information: This work was supported by the National Institutes of Health , the National Institute of Neurological Disorders and Stroke [ NS40068 to J.S.P.] and the CHDI Foundation, Inc. We thank the PREDICT-HD sites, the study participants, and the National Research Roster for Huntington Disease Patients and Families.
PY - 2012/6
Y1 - 2012/6
N2 - Leukocyte 8-hydroxydeoxyguanosine (8OHdG) is an indicator of oxidative stress, impaired metabolism, and mitochondrial dysfunction, features that have been implicated in Huntington disease (HD). Increased levels of 8OHdG have been reported in the caudate, parietal cortex, and peripherally in the serum and leukocytes, in patients diagnosed with HD. However, little is known about levels in prodromal patients and changes that might occur as the disease progresses. To address these issues, 8OHdG was tracked over time for a subset of participants enrolled in the PREDICT-HD study. Participants were stratified into four groups based on proximity to HD diagnosis at study entry: Controls (gene-negative individuals), Low (low probability of near-future diagnosis), Medium, and High. Blood samples were analyzed using Liquid Chromatography Electrochemical Array, and for comparison purposes, a separate cross-sectional sample was analyzed using liquid chromatography coupled with multiple-reaction-monitoring mass spectrometry. Longitudinal data analysis showed that initial status (at study entry) and annual rate of change varied as a function of proximity group, adjusting for sex, education, age at study entry, and site effects. Overall levels were lowest for the Control group and highest for the High group, and the rate of increase varied in a similar manner. The finding that 8OHdG concentrations increased as a function of proximity to projected disease diagnosis and duration indicates support for the continued assessment of 8OHdG as a robust clinical HD biomarker.
AB - Leukocyte 8-hydroxydeoxyguanosine (8OHdG) is an indicator of oxidative stress, impaired metabolism, and mitochondrial dysfunction, features that have been implicated in Huntington disease (HD). Increased levels of 8OHdG have been reported in the caudate, parietal cortex, and peripherally in the serum and leukocytes, in patients diagnosed with HD. However, little is known about levels in prodromal patients and changes that might occur as the disease progresses. To address these issues, 8OHdG was tracked over time for a subset of participants enrolled in the PREDICT-HD study. Participants were stratified into four groups based on proximity to HD diagnosis at study entry: Controls (gene-negative individuals), Low (low probability of near-future diagnosis), Medium, and High. Blood samples were analyzed using Liquid Chromatography Electrochemical Array, and for comparison purposes, a separate cross-sectional sample was analyzed using liquid chromatography coupled with multiple-reaction-monitoring mass spectrometry. Longitudinal data analysis showed that initial status (at study entry) and annual rate of change varied as a function of proximity group, adjusting for sex, education, age at study entry, and site effects. Overall levels were lowest for the Control group and highest for the High group, and the rate of increase varied in a similar manner. The finding that 8OHdG concentrations increased as a function of proximity to projected disease diagnosis and duration indicates support for the continued assessment of 8OHdG as a robust clinical HD biomarker.
KW - 8OHdG
KW - Biomarker
KW - Huntington disease
KW - Mitochondrial dysfunction
KW - Oxidative stress
KW - PREDICT-HD
UR - http://www.scopus.com/inward/record.url?scp=84860835246&partnerID=8YFLogxK
U2 - 10.1016/j.nbd.2012.02.012
DO - 10.1016/j.nbd.2012.02.012
M3 - Article
C2 - 22414782
AN - SCOPUS:84860835246
SN - 0969-9961
VL - 46
SP - 625
EP - 634
JO - Neurobiology of Disease
JF - Neurobiology of Disease
IS - 3
ER -