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Biomarkers of Oral Inflammation in Perinatally HIV-infected and Perinatally HIV-exposed, Uninfected Youth.

Anna-Barbara Moscicki,Tzy-Jyun Yao,Jonathan S. Russell,Sepideh Farhat,Mark Scott,Larry Magpantay,Gordana Halec,Caroline H. Shiboski,Mark Ryder, Ester Yang, William Shearer, Mary Paul, Norma Cooper, Lynette Harris, Karen Kemp-Posterman, Selene Wun, Murli Purswani, Mahboobullah Baig, Anna Cintron, Jennifer Zeni, Ana Puga, Sandra Navarro, Doyle Patton, Deyana Leon, Man Wai Ng, Sandra Burchett, Nancy Karthas, Betsy Kammerer, Ray Jurado, Johnny Kuttab, Ashlee Vorachek, Ram Yogev, Margaret Ann Sanders, Kathleen Malee, Scott Hunter, Victor Badner, Ronald Garreett, Andrew Wiznia, Marlene Burey, Molly Nozyce, Susan Chialastri, Janet Chen, Latreca Ivey, Maria Garcia Bulkley, Mitzie Grant, Ramon Gonzalez, Midnela Acevedo-Flores, Heida Rios, Vivian Olivera, Janice Townsend, Margarita Silio, Medea Jones, Patricia Sirois, Roopa Gandhi, Elizabeth McFarland, Emily Barr, Robin McEvoy, Kenneth Markowitz, Arry Dieudonne, Linda Bettica, Susan Adubato

Journal of clinical periodontology(2019)

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摘要
Aim To examine oral biomarkers that have been associated with periodontal disease progression in HIV-infected adults in perinatally HIV-infected and HIV-exposed but uninfected youth. Material and Methods This was a cross-sectional, multicentre substudy of youth participating in the Oral Health Pediatric HIV/AIDS Cohort study. Gingival crevicular fluid repository samples from participants with and without periodontal disease (using Gingival Index [GI] and Bleeding on Probing [BOP] parameters on dental examination) were tested for concentration levels of inflammatory biomarkers. Associations were assessed using Wilcoxon test and Spearman correlation. Results For perinatal HIV youth (n = 129), the markers consistently elevated (p < .05) in sites with GI >= 2 and in sites with BOP were interleukin-1 beta, 6 and 13, macrophage inflammatory protein-1 alpha and metalloproteinase-9. Serum tumour necrosis factor-alpha and soluble CD14 were positively correlated with a summary count of elevated cytokines. No associations were seen among HIV-uninfected subjects (n = 71). Conclusions The association of oral biomarkers of inflammation with clinical indicators of periodontal inflammation and systemic immune activation suggests that perinatal HIV-infected youth may be at higher risk for developing significant periodontal disease, associated with tooth loss and HIV progression. More frequent dental care of this group is needed to prevent potential periodontal progression.
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关键词
cytokines,oral health,perinatal HIV-infected youth,periodontal inflammation
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