| BMC Infectious Diseases | |
| Pre-vaccination type-specific HPV prevalence in confirmed cervical high grade lesions in the Māori and non-Māori populations in New Zealand | |
| Research Article | |
| Leonardo Simonella1 Collette Bromhead2 Harold Neal3 Hazel Lewis4 Karen Canfell5 Yoon-Jung Kang5 Megan A. Smith5 | |
| [1] Cancer Research Division, Cancer Council NSW, 153 Dowling Street, 2011, Woolloomooloo, NSW, Australia;Current address: MORSE (modelling outcomes research, statistics and epidemiology) group, Roche, Basel, Switzerland;Molecular Biology, Aotea Pathology, CMC Building 89 Courtenay Place, Wellington, New Zealand;Current address: Institute of Food and Nutrition, College of Health, Massey University Wellington, Wellington, New Zealand;National Cervical Screening Programme, Ministry of Health, Wellington, New Zealand;National Cervical Screening Programme, Ministry of Health, Wellington, New Zealand;Current address: 59 Normandale Rd, Lower Hutt, New Zealand;Prince of Wales Clinical School, UNSW, 2052, Sydney, NSW, Australia;Cancer Research Division, Cancer Council NSW, 153 Dowling Street, 2011, Woolloomooloo, NSW, Australia; | |
| 关键词: Indigenous populations; HPV vaccine; Vaccine impact; Cervical cancer; New Zealand; | |
| DOI : 10.1186/s12879-015-1034-5 | |
| received in 2015-01-30, accepted in 2015-07-16, 发布年份 2015 | |
| 来源: Springer | |
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【 摘 要 】
BackgroundNew Zealand initiated HPV vaccination in 2008, and has attained 3-dose coverage of ~50 % in 12–13 year old girls. Due to the success of program initiatives in Māori girls, higher coverage rates of ~60 % have been achieved in this group. We have previously reported a benchmark overall pre-vaccination prevalence of oncogenic HPV infection in high grade cervical lesions in New Zealand. The current extended analysis provides separate pre-vaccination benchmark prevalence for Māori and non-Māori women.MethodsThe National Cervical Screening Programme Register (NCSP-R) was used to identify any woman aged 20–69 years of age with an index high grade cytology report from 2009–2011. Extended recruitment was performed until 2012 in clinics with a high proportion of Māori women. Ethnicity status was based on self-reported information by participating women through phone contact supplemented by recordings on the study questionnaire (the NCSP-R was not used to extract ethnicity status). A total of 730 women consented to participate and had a valid HPV test result; 418 of these had histologically-confirmed cervical intraepithelial neoplasia (CIN) 2/3 lesions (149 Māori, 269 non-Māori). The prevalence of any cervical oncogenic HPV infection, HPV16, and HPV18 was calculated in women with CIN2/3.ResultsIn confirmed CIN2/3, the prevalence of any oncogenic HPV, HPV16 and HPV18 was 96 % (95 % CI:91–99 %), 54 % (95 % CI:46–63 %), 11 % (95 % CI:7–18 %) in Māori and 96 % (95 % CI:93–98 %), 54 % (95 % CI:48–60 %), 11 % (95 % CI:7–15 %) in non-Māori women, respectively. Age-specific patterns of infection for HPV16/18 in confirmed CIN2/3 differed between the two groups (Pinteraction = 0.02), with a lower prevalence in younger vs. older Māori women (57 % in 20–29 years vs 75 % in 40–69 years) but a higher prevalence in younger vs. older non-Māori women (70 % in 20–29 years vs 49 % in 40–69 years); the difference in the age-specific patterns of infection for HPV16/18 was not significant either when considering confirmed CIN2 alone (p = 0.09) or CIN3 alone (p = 0.22).ConclusionsThe overall prevalence of vaccine-included types in CIN2/3 was similar in Māori and non-Māori women, implying that the long-term effects of vaccination will be similar in the two groups.
【 授权许可】
CC BY
© Kang et al. 2015
【 预 览 】
| Files | Size | Format | View |
|---|---|---|---|
| RO202311107654905ZK.pdf | 989KB |  download |
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