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Racial and ethnic disparities in human papillomavirus‐associated cancer burden with first‐generation and second‐generation human papillomavirus vaccines
Author(s) -
Burger Emily A.,
Lee Kyueun,
Saraiya Mona,
Thompson Trevor D.,
Chesson Harrell W.,
Markowitz Lauri E.,
Kim Jane J.
Publication year - 2016
Publication title -
cancer
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 3.052
H-Index - 304
eISSN - 1097-0142
pISSN - 0008-543X
DOI - 10.1002/cncr.30007
Subject(s) - medicine , ethnic group , vaccination , cervical cancer , human papillomavirus , cancer , demography , incidence (geometry) , epidemiology , health equity , hpv vaccines , hpv infection , immunology , public health , pathology , physics , sociology , anthropology , optics
BACKGROUND In the United States, the burden of human papillomavirus (HPV)‐associated cancers varies by racial/ethnic group. HPV vaccination may provide opportunities for primary prevention of these cancers. Herein, the authors projected changes in HPV‐associated cancer burden among racial/ethnic groups under various coverage assumptions with the available first‐generation and second‐generation HPV vaccines to evaluate changes in racial/ethnic disparities. METHODS Cancer‐specific mathematical models simulated the burden of 6 HPV‐associated cancers. Model parameters, informed using national registries and epidemiological studies, reflected sex‐specific, age‐specific, and racial/ethnic‐specific heterogeneities in HPV type distribution, cancer incidence, stage of disease at detection, and mortality. Model outcomes included the cumulative lifetime risks of developing and dying of 6 HPV‐associated cancers. The level of racial/ethnic disparities was evaluated under each alternative HPV vaccine scenario using several metrics of social group disparity. RESULTS HPV vaccination is expected to reduce the risks of developing and dying of HPV‐associated cancers in all racial/ethnic groups as well as reduce the absolute degree of disparities. However, alternative metrics suggested that relative disparities would persist and in some scenarios worsen. For example, when assuming high uptake with the second‐generation HPV vaccine, the lifetime risk of dying of an HPV‐associated cancer for males decreased by approximately 60%, yet the relative disparity increased from 3.0 to 3.9. CONCLUSIONS HPV vaccines are expected to reduce the overall burden of HPV‐associated cancers for all racial/ethnic groups and to reduce the absolute disparity gap. However, even with the second‐generation vaccine, relative disparities will likely still exist and may widen if the underlying causes of these disparities remain unaddressed. Cancer 2016;122:2057–66 . © 2016 American Cancer Society .

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