Noonan 综合征中循环造血祖细胞的功能评估。
Functional evaluation of circulating hematopoietic progenitors in Noonan syndrome.
机构信息
Pediatric Hematology-Oncology, Regina Margherita Children's Hospital, 10126 Turin, Italy.
出版信息
Oncol Rep. 2013 Aug;30(2):553-9. doi: 10.3892/or.2013.2535. Epub 2013 Jun 11.
Noonan syndrome (NS) is an autosomal dominant disorder, characterized by short stature, multiple dysmorphisms and congenital heart defects. A myeloproliferative disorder (NS/MPD), resembling juvenile myelomonocytic leukemia (JMML), is occasionally diagnosed in infants with NS. In the present study, we performed a functional evaluation of the circulating hematopoietic progenitors in a series of NS, NS/MPD and JMML patients. The different functional patterns were compared with the aim to identify a possible NS subgroup worthy of stringent hematological follow-up for an increased risk of MPD development. We studied 27 NS and 5 JMML patients fulfilling EWOG-MDS criteria. The more frequent molecular defects observed in NS were mutations in the PTPN11 and SOS genes. The absolute count of monocytes, circulating CD34+ hematopoietic progenitors, their apoptotic rate and the number of circulating CFU-GMs cultured in the presence of decreasing concentrations or in the absence of granulocyte-macrophage colony-stimulating factor (GM-CSF) were evaluated. All JMML patients showed monocytosis>1,000/µl. Ten out of the 27 NS patients showed monocytosis>1,000/µl, which included the 3 NS/MPD patients. In JMML patients, circulating CD34+ cells were significantly increased (median, 109.8/µl; range, 44-232) with a low rate of apoptosis (median, 2.1%; range, 0.4-12.1%), and circulating CFU-GMs were hyper-responsive to GM-CSF. NS/MPD patients showed the same flow cytometric pattern as the JMML patients (median, CD34+ cells/µl, 205.7; range, 58-1374; median apoptotic rate, 1.4%; range, 0.2-2.4%) and their circulating CFU-GMs were hyper-responsive to GM-CSF. These functional alterations appeared 10 months before the typical clinical manifestations in 1 NS/MPD patient. In NS, the CD34+ absolute cell count and circulating CFU-GMs showed a normal pattern (median CD34+ cells/µl, 4.9; range, 1.3-17.5), whereas the CD34+ cell apoptotic rate was significantly decreased in comparison with the controls (median, 8.6%; range, 0-27.7% vs. median, 17.6%; range, 2.8-49.6%), suggesting an increased CD34+ cell survival. The functional evaluation of circulating hematopoietic progenitors showed specific patterns in NS and NS/MPD. These tests are a reliable integrative tool that, together with clinical data and other hematological parameters, could help detect NS patients with a high risk for a myeloproliferative evolution.
努南综合征(Noonan syndrome,NS)是一种常染色体显性遗传疾病,其特征为身材矮小、多种畸形和先天性心脏病。在婴儿中,偶尔会诊断出具有 NS 的髓系增生性疾病(NS/MPD),类似于幼年髓单核细胞白血病(juvenile myelomonocytic leukemia,JMML)。在本研究中,我们对一系列 NS、NS/MPD 和 JMML 患者的循环造血祖细胞进行了功能评估。我们将不同的功能模式进行了比较,旨在确定一个可能的 NS 亚组,该亚组值得进行严格的血液学随访,以增加 MPD 发展的风险。我们研究了 27 名符合 EWOG-MDS 标准的 NS 和 5 名 JMML 患者。在 NS 中观察到的更常见的分子缺陷是 PTPN11 和 SOS 基因的突变。我们评估了循环单核细胞、循环 CD34+造血祖细胞的绝对计数、其凋亡率以及在降低浓度或缺乏粒细胞-巨噬细胞集落刺激因子(granulocyte-macrophage colony-stimulating factor,GM-CSF)的情况下培养的循环 CFU-GM 的数量。所有 JMML 患者均表现为单核细胞计数>1000/µl。27 名 NS 患者中有 10 名表现为单核细胞计数>1000/µl,其中包括 3 名 NS/MPD 患者。JMML 患者的循环 CD34+细胞明显增加(中位数,109.8/µl;范围,44-232),凋亡率较低(中位数,2.1%;范围,0.4-12.1%),并且循环 CFU-GM 对 GM-CSF 反应过度。NS/MPD 患者表现出与 JMML 患者相同的流式细胞术模式(中位数 CD34+细胞/µl,205.7;范围,58-1374;中位数凋亡率,1.4%;范围,0.2-2.4%),其循环 CFU-GM 对 GM-CSF 反应过度。在 1 名 NS/MPD 患者中,这些功能改变在典型临床表现出现前 10 个月就已经出现。在 NS 中,CD34+绝对细胞计数和循环 CFU-GM 表现出正常模式(中位数 CD34+细胞/µl,4.9;范围,1.3-17.5),而 CD34+细胞凋亡率与对照组相比显著降低(中位数,8.6%;范围,0-27.7% vs. 中位数,17.6%;范围,2.8-49.6%),提示 CD34+细胞的存活增加。循环造血祖细胞的功能评估显示 NS 和 NS/MPD 具有特定的模式。这些测试是一种可靠的综合工具,与临床数据和其他血液学参数一起,可帮助检测具有髓系增生演变高风险的 NS 患者。
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