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特立帕肽(PTH 1-34)治疗可增加绝经后妇女外周造血干细胞。

Teriparatide (PTH 1-34) treatment increases peripheral hematopoietic stem cells in postmenopausal women.

机构信息

Endocrine Unit, Massachusetts General Hospital, Boston, MA, USA.

出版信息

J Bone Miner Res. 2014 Jun;29(6):1380-6. doi: 10.1002/jbmr.2171.

Abstract

Cells of the osteoblast lineage play an important role in regulating the hematopoietic stem cell (HSC) niche and early B-cell development in animal models, perhaps via parathyroid hormone (PTH)-dependent mechanisms. There are few human clinical studies investigating this phenomenon. We studied the impact of long-term daily teriparatide (PTH 1-34) treatment on cells of the hematopoietic lineage in postmenopausal women. Twenty-three postmenopausal women at high risk of fracture received teriparatide 20 mcg sc daily for 24 months as part of a prospective longitudinal trial. Whole blood measurements were obtained at baseline, 3, 6, 12, and 18 months. Flow cytometry was performed to identify hematopoietic subpopulations, including HSCs (CD34+/CD45(moderate); ISHAGE protocol) and early transitional B cells (CD19+, CD27-, IgD+, CD24[hi], CD38[hi]). Serial measurements of spine and hip bone mineral density (BMD) as well as serum P1NP, osteocalcin, and CTX were also performed. The average age of study subjects was 64 ± 5 years. We found that teriparatide treatment led to an early increase in circulating HSC number of 40% ± 14% (p = 0.004) by month 3, which persisted to month 18 before returning to near baseline by 24 months. There were no significant changes in transitional B cells or total B cells over the course of the study period. In addition, there were no differences in complete blood count profiles as quantified by standard automated flow cytometry. Interestingly, the peak increase in HSC number was inversely associated with increases in bone markers and spine BMD. Daily teriparatide treatment for osteoporosis increases circulating HSCs by 3 to 6 months in postmenopausal women. This may represent a proliferation of marrow HSCs or increased peripheral HSC mobilization. This clinical study establishes the importance of PTH in the regulation of the HSC niche within humans. © 2014 American Society for Bone and Mineral Research.

摘要

成骨细胞系细胞在调节动物模型中的造血干细胞(HSC)龛和早期 B 细胞发育方面发挥着重要作用,这可能是通过甲状旁腺激素(PTH)依赖的机制。目前很少有研究人类的临床研究调查这种现象。我们研究了长期每日特立帕肽(PTH 1-34)治疗对绝经后妇女造血谱系细胞的影响。23 名有骨折高风险的绝经后妇女作为前瞻性纵向试验的一部分,每天接受特立帕肽 20 mcg sc 治疗 24 个月。在基线、3、6、12 和 18 个月时获得全血测量值。通过流式细胞术鉴定造血亚群,包括 HSCs(CD34+/CD45(moderate);ISHAGE 方案)和早期过渡 B 细胞(CD19+,CD27-,IgD+,CD24[高],CD38[高])。还进行了脊柱和髋部骨密度(BMD)以及血清 P1NP、骨钙素和 CTX 的连续测量。研究对象的平均年龄为 64±5 岁。我们发现,特立帕肽治疗在 3 个月时导致循环 HSC 数量早期增加 40%±14%(p=0.004),并持续到 18 个月,然后在 24 个月时恢复到接近基线。在研究期间,过渡 B 细胞或总 B 细胞没有明显变化。此外,通过标准自动化流式细胞术定量的全血细胞谱没有差异。有趣的是,HSC 数量的峰值增加与骨标志物和脊柱 BMD 的增加呈负相关。骨质疏松症的每日特立帕肽治疗可使绝经后妇女的循环 HSC 在 3 至 6 个月内增加。这可能代表骨髓 HSC 的增殖或外周 HSC 动员的增加。这项临床研究确立了 PTH 在调节人类 HSC 龛中的重要性。

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