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通过坦桑尼亚的零售药店扩大基于寄生虫的疟疾诊断服务:一项随机试验的证据及其对治疗的影响

Expanding access to parasite-based malaria diagnosis through retail drug shops in Tanzania: evidence from a randomized trial and implications for treatment.

作者信息

Maloney Kathleen, Ward Abigail, Krenz Bonnie, Petty Nora, Bryson Lindsay, Dolkart Caitlin, Visser Theodoor, Le Menach Arnaud, Scott Valerie K, Cohen Justin M, Mtumbuka Esther, Mkude Sigsbert

机构信息

Clinton Health Access Initiative, Inc., 383 Dorchester Avenue Suite 400, Boston, MA, 02127, USA.

Clinton Health Access Initiative, Inc., Tanzania Office, Dar es Salaam, Tanzania.

出版信息

Malar J. 2017 Jan 3;16(1):6. doi: 10.1186/s12936-016-1658-y.

Abstract

BACKGROUND

Tanzania has seen a reduction in the fraction of fevers caused by malaria, likely due in part to scale-up of control measures. While national guidelines require parasite-based diagnosis prior to treatment, it is estimated that more than half of suspected malaria treatment-seeking in Tanzania initiates in the private retail sector, where diagnosis by malaria rapid diagnostic test (RDT) or microscopy is illegal. This pilot study investigated whether the introduction of RDTs into Accredited Drug Dispensing Outlets (ADDOs) under realistic market conditions would improve case management practices.

METHODS

Dispensers from ADDOs in two intervention districts in Tanzania were trained to stock and perform RDTs and monitored quarterly. Each district was assigned a different recommended retail price to evaluate the need for a subsidy. Malaria RDT and artemisinin-based combination therapy (ACT) uptake and availability were measured pre-intervention and 1 year post-intervention through structured surveys of ADDO owners and exiting customers in both intervention districts and one contiguous control district. Descriptive analysis and logistic regression were used to compare the three districts and identify predictive variables for testing.

RESULTS AND DISCUSSION

A total of 310 dispensers from 262 ADDOs were trained to stock and perform RDTs. RDT availability in intervention ADDOs increased from 1% (n = 172) to 73% (n = 163) during the study; ACT medicines were available in 75% of 260 pre-intervention and 68% of 254 post-intervention ADDOs. Pre-treatment testing performed within the ADDO increased from 0 to 65% of suspected malaria patients who visited a shop (95% CI 60.8-69.6%) with no difference between intervention districts. Overall parasite-based diagnosis increased from 19 to 74% in intervention districts and from 3 to 18% in the control district. Prior knowledge of RDT availability (aOR = 1.9, p = 0.03) and RDT experience (aOR = 1.9, p = 0.01) were predictors for testing. Adherence data indicated that 75% of malaria positives received ACT, while 3% of negatives received ACT.

CONCLUSIONS

Trained and supervised ADDO dispensers in rural Tanzania performed and sold RDTs under real market conditions to two-thirds of suspected malaria patients during this one-year pilot. These results support the hypothesis that introducing RDTs into regulated private retail sector settings can improve malaria testing and treatment practices without an RDT subsidy. Trial registration ISRCTN ISRCTN14115509.

摘要

背景

坦桑尼亚因疟疾导致的发热比例有所下降,这可能部分归因于防控措施的扩大实施。虽然国家指南要求在治疗前进行基于寄生虫的诊断,但据估计,坦桑尼亚超过一半寻求疟疾治疗的疑似患者是在私营零售部门开始治疗的,而在该部门通过疟疾快速诊断检测(RDT)或显微镜进行诊断是违法的。这项试点研究调查了在现实市场条件下,将RDT引入经认证的药品零售点(ADDO)是否会改善病例管理实践。

方法

对坦桑尼亚两个干预地区的ADDO药剂师进行培训,使其储备并开展RDT检测,并每季度进行监测。为每个地区设定不同的建议零售价,以评估补贴的必要性。通过对两个干预地区和一个相邻对照地区的ADDO店主及离开的顾客进行结构化调查,在干预前和干预后1年测量疟疾RDT和基于青蒿素的联合疗法(ACT)的使用情况和可获得性。采用描述性分析和逻辑回归来比较这三个地区,并确定检测的预测变量。

结果与讨论

来自262个ADDO的310名药剂师接受了储备和开展RDT检测的培训。在研究期间,干预地区ADDO的RDT可获得性从1%(n = 172)增至73%(n = 163);260个干预前ADDO中有75%可获得ACT药物,254个干预后ADDO中有68%可获得。在ADDO内进行的治疗前检测从0增至到店的疑似疟疾患者的65%(95%可信区间60.8 - 69.6%),干预地区之间无差异。干预地区基于寄生虫的总体诊断从19%增至74%,对照地区从3%增至18%。RDT可获得性的先验知识(校正比值比 = 1.9,p = 0.03)和RDT经验(校正比值比 = 1.9,p = 0.01)是检测的预测因素。依从性数据表明,75%的疟疾阳性患者接受了ACT治疗,而3%的阴性患者接受了ACT治疗。

结论

在这为期一年的试点期间,坦桑尼亚农村地区经过培训和监督的ADDO药剂师在实际市场条件下,为三分之二的疑似疟疾患者开展并销售了RDT检测。这些结果支持了以下假设:在无RDT补贴的情况下,将RDT引入受监管的私营零售部门环境可改善疟疾检测和治疗实践。试验注册号:ISRCTN ISRCTN14115509 。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1ab6/5209819/f71c6d39bca3/12936_2016_1658_Fig1_HTML.jpg

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