Drugs for Neglected Diseases initiative (DNDi), New York, United States of America.
Division of Clinical Medicine, Rajendra Memorial Research Institute of Medical Sciences (RMRI), Patna, Bihar, India.
PLoS Negl Trop Dis. 2020 Jul 20;14(7):e0008429. doi: 10.1371/journal.pntd.0008429. eCollection 2020 Jul.
Few prospective data exist on incidence of post kala-azar dermal leishmaniasis (PKDL) and visceral leishmaniasis (VL) relapse after different treatment regimens.
METHODOLOGY/PRINCIPAL FINDINGS: A Phase IV trial included 1761 VL patients treated between 2012-2014 with single dose AmBisome (SDA; N = 891), miltefosine-paromomycin (Milt-PM; n = 512), or AmBisome-miltefosine (AmB-Milt; n = 358). Follow-up for PKDL and VL relapse was scheduled for 6, 12 and 24 months after treatment, lasting until 2017. Patients with lesions consistent with PKDL were tested by rK39 rapid test, and if positive, underwent skin-snip sampling, smear microscopy and PCR. Probable PKDL was defined by consistent lesions and positive rK39; confirmed PKDL required additional positive microscopy or PCR. PKDL and relapse incidence density were calculated by VL treatment and risk factors evaluated in Cox proportional hazards models. Among 1,750 patients who completed treatment, 79 had relapse and 104 PKDL. Relapse incidence density was 1.58, 2.08 and 0.40 per 1000 person-months for SDA, AmB-Milt and Milt-PM, respectively. PKDL incidence density was 1.29, 1.45 and 2.65 per 1000 person-months for SDA, AmB-Milt and Milt-PM. In multivariable models, patients treated with Milt-PM had lower relapse but higher PKDL incidence than those treated with SDA; AmB-Milt rates were not significantly different from those for SDA. Children <12 years were at higher risk for both outcomes; females had a higher risk of PKDL but not relapse.
CONCLUSIONS/SIGNIFICANCE: Active surveillance for PKDL and relapse, followed by timely treatment, is essential to sustain the achievements of VL elimination programs in the Indian sub-continent.
关于不同治疗方案后出现的黑热病后皮肤利什曼病(PKDL)和内脏利什曼病(VL)复发的发生率,目前仅有少量前瞻性数据。
方法/主要发现:一项 4 期试验纳入了 1761 例 2012-2014 年期间接受单剂量两性霉素 B 脂质体(SDA;N=891)、米替福新-硫酸巴龙霉素(Milt-PM;n=512)或两性霉素 B-米替福新(AmB-Milt;n=358)治疗的 VL 患者。治疗后第 6、12 和 24 个月计划进行 PKDL 和 VL 复发随访,随访持续到 2017 年。对符合 PKDL 的病变患者进行 rK39 快速检测,如果阳性,则进行皮肤活检、涂片显微镜检查和 PCR。疑似 PKDL 通过一致的病变和阳性 rK39 定义;确诊 PKDL 需要额外的显微镜检查或 PCR 阳性。通过 VL 治疗和 Cox 比例风险模型评估的风险因素计算 PKDL 和复发发生率密度。在完成治疗的 1750 例患者中,79 例出现复发,104 例出现 PKDL。SDA、AmB-Milt 和 Milt-PM 的复发发生率密度分别为每 1000 人月 1.58、2.08 和 0.40;PKDL 发生率密度分别为每 1000 人月 1.29、1.45 和 2.65。在多变量模型中,与 SDA 相比,接受 Milt-PM 治疗的患者复发率较低,但 PKDL 发生率较高;AmB-Milt 的发生率与 SDA 无显著差异。<12 岁的儿童两种结局的风险较高;女性 PKDL 的风险较高,但复发风险无差异。
结论/意义:对 PKDL 和复发进行主动监测,并及时进行治疗,对于维持南亚次大陆消除 VL 规划的成果至关重要。
