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中性粒细胞与淋巴细胞比值作为真性红细胞增多症中JAK2抑制和无事件生存期的替代指标。

Neutrophil-to-Lymphocyte ratio as surrogate for JAK2 suppression and event-free survival in polycythemia vera.

作者信息

Barbui Tiziano, Ghirardi Arianna, Empson Victoria, Fenili Francesca, Loscocco Giuseppe Gaetano, Condorelli Annalisa, Iurlo Alessandra, Cattaneo Daniele, Rossi Elena, De Stefano Valerio, Guglielmelli Paola, Klade Christoph, Gisslinger Heinz, Rambaldi Alessandro, Scandura Joseph M, Vannucchi Alessandro Maria

机构信息

FROM, Fondazione per la Ricerca Ospedale di Bergamo ETS, Bergamo, Italy.

AOP Orphan Pharmaceuticals GmbH, Vienna, Austria.

出版信息

Blood Cancer J. 2025 Aug 6;15(1):132. doi: 10.1038/s41408-025-01317-6.

Abstract

Chronic systemic inflammation is a key driver of polycythemia vera (PV) progression, but the immunomodulatory effects of current treatments remain poorly defined. The neutrophil-to-lymphocyte ratio (NLR) is an accessible biomarker of systemic inflammation proven in other contexts, but its role in monitoring PV disease activity has not been established. Using data from three of the largest PV clinical trials, we evaluated the effects of PV therapies on NLR and its relationship with molecular response and clinical outcomes. In 404 hematocrit-controlled patients from the ECLAP study, hydroxyurea (HU) failed to significantly lower NLR (p = 0.11) due to the parallel declines in ANC and ALC. Neither leukocyte counts nor NLR were significantly reduced by phlebotomy in ECLAP patients treated without cytoreductive therapy. In contrast, the Low-PV study showed that while phlebotomy tended to increase NLR, low-dose ropeginterferon alfa-2b (Ropeg) significantly reduced NLR (-18.2% and -36.3% in patients with low and high baseline NLR, respectively) by suppressing ANC rather than lymphocytes. NLR reduction correlated with the primary Low-PV endpoint (p = 0.021) and reduction of JAK2 variant allele frequency (VAF) [1]. The PROUD-PV/CONTINUATION-PV study confirmed the superior effect of Ropeg over HU, with a significantly greater NLR reduction at 60 months (-56.5% versus -33.6%, respectively, p = 0.019) in patients with high baseline NLR. Moreover, NLR reduction was associated with decreased JAK2 VAF (p < 0.0001) and improved event-free survival (p = 0.010). These findings identify NLR as a dynamic biomarker of treatment response and prognosis in PV and support its incorporation into routine monitoring.

摘要

慢性全身性炎症是真性红细胞增多症(PV)进展的关键驱动因素,但目前治疗的免疫调节作用仍不明确。中性粒细胞与淋巴细胞比值(NLR)是在其他情况下已得到证实的全身性炎症的一个可获取的生物标志物,但其在监测PV疾病活动中的作用尚未确立。利用来自三项最大的PV临床试验的数据,我们评估了PV疗法对NLR的影响及其与分子反应和临床结局的关系。在ECLAP研究的404例血细胞比容得到控制的患者中,由于中性粒细胞绝对值(ANC)和淋巴细胞绝对值(ALC)同时下降,羟基脲(HU)未能显著降低NLR(p = 0.11)。在未接受细胞减灭治疗的ECLAP患者中,放血疗法既未显著降低白细胞计数,也未显著降低NLR。相比之下,Low-PV研究表明,虽然放血疗法往往会使NLR升高,但低剂量聚乙二醇化干扰素α-2b(Ropeg)通过抑制ANC而非淋巴细胞,显著降低了NLR(基线NLR低和高的患者分别降低了18.2%和36.3%)。NLR降低与Low-PV研究的主要终点相关(p = 0.021)以及JAK2变异等位基因频率(VAF)降低相关[1]。PROUD-PV/CONTINUATION-PV研究证实了Ropeg优于HU,在基线NLR高的患者中,60个月时NLR降低幅度显著更大(分别为-56.5%和-33.6%,p = 0.019)。此外,NLR降低与JAK2 VAF降低相关(p < 0.0001)且无事件生存期改善(p = 0.010)。这些发现确定NLR是PV治疗反应和预后的动态生物标志物,并支持将其纳入常规监测。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4c76/12328675/75d1a0ba6a3e/41408_2025_1317_Fig1_HTML.jpg

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