Del Cañizo M C, Galende J, Mota A, Orfao A, Martinez A, Almeida J, San Miguel J F
Servicio de Hematología Hospital Universitario, Salamanca, Spain.
Leuk Res. 1997 Jul;21(7):651-6. doi: 10.1016/s0145-2126(97)00031-3.
The aim of the present study was to analyze whether or not leukemic clonogenic cells are restricted to the CD34+ cell fraction and to investigate the effect of IL-3 and G-CSF on blast cell populations dissected according to their CD34 reactivity. For this purpose 34 patients were studied. Patients were classified into three groups according to CD34 antigen expression: (1) cases in which all blast cells (100%) were positive for the CD34 Ag (n = 9); (2) cases in which all blast cells lacked the expression of this antigen (n = 10); and (3) patients in whom both, CD34 positive and negative blast cell subsets coexisted (n = 15). In 15 cases immunomagnetic cell selection was performed and two subpopulations were separated: one, phenotypically more immature (CD34+), and another, theoretically more differentiated (CD34-/33+). In addition, in three cases both CD34+ and CD34- blast cell subpopulations were sorted using a FACStar flow cytometer. Blast colony assays were performed using 0.9% methylcellulose and two different recombinant human hematopoietic growth factors (HGFs), IL-3 and G-CSF, were used as growth stimulants. Either, a single or a combination of the growth factors was added to cultures. Colony formation was observed in both 100% positive or 100% negative cases for the CD34 antigen as well as in the CD34+ and CD34- cell fractions separated by immunomagnetic selection or flow cytometry. The effect of G-CSF and IL-3 on both cell fractions was as follows: cases with a uniform population according to CD34 expression (100% positive or negative) showed a better growth response with IL-3 especially for the CD34+ cases (87% vs 40% of CD34+ and CD34- cases, respectively). Within the CD34-/33+ selected fractions, IL-3 tended to induce a higher proliferative response than G-CSF while the opposite was found within the CD34+ cell selected fractions. In contrast it was observed that both IL-3 and G-CSF induced a higher PE on the CD34- blast cells (both selected and 100% negative), although the difference was not statistically significant. The existence of a possible synergistic effect (SE) between HGFs was also explored. Overall, a synergistic growth was observed in nine out of the 13 selected cases studied and this effect could be seen in both CD34- or CD34+ blast cell fractions. The analysis of the complete phenotypic characteristics of these cells revealed that cell fractions showing SE were more immature according to the expression of CD15 and HLA-DR antigens. We can conclude that in leukemic hematopoiesis, CD34 antigen expression does not have the same significance as it does in normal hematopoiesis since clonogenic cells are not restricted to the CD34+ acute myeloid leukemia (AML) blast cell fraction. Moreover, our study shows that the heterogeneous response to HGFs observed in AML patients may be associated with the existence of immunophenotypically different blast cell subsets.
本研究的目的是分析白血病克隆形成细胞是否仅限于CD34+细胞部分,并研究白细胞介素-3(IL-3)和粒细胞集落刺激因子(G-CSF)对根据其CD34反应性分离的原始细胞群体的影响。为此,对34例患者进行了研究。根据CD34抗原表达将患者分为三组:(1)所有原始细胞(100%)CD34抗原阳性的病例(n = 9);(2)所有原始细胞均缺乏该抗原表达的病例(n = 10);(3)CD34阳性和阴性原始细胞亚群共存的患者(n = 15)。在15例病例中进行了免疫磁珠细胞分选,分离出两个亚群:一个在表型上更不成熟(CD34+),另一个理论上更分化(CD34-/33+)。此外,在3例病例中,使用FACStar流式细胞仪对CD34+和CD34-原始细胞亚群进行了分选。使用0.9%甲基纤维素进行原始细胞集落测定,并使用两种不同的重组人造血生长因子(HGFs),即IL-3和G-CSF作为生长刺激剂。将单一或组合的生长因子添加到培养物中。在CD34抗原100%阳性或100%阴性的病例以及通过免疫磁珠分选或流式细胞术分离的CD34+和CD34-细胞部分中均观察到集落形成。G-CSF和IL-3对这两个细胞部分的影响如下:根据CD34表达具有均匀群体的病例(100%阳性或阴性)对IL-3显示出更好的生长反应,特别是对于CD34+病例(分别为CD34+和CD34-病例的87%和40%)。在CD34-/33+分选部分中,IL-3倾向于比G-CSF诱导更高的增殖反应,而在CD34+细胞分选部分中则相反。相反,观察到IL-3和G-CSF均在CD34-原始细胞(分选的和100%阴性的)上诱导更高的增殖效应,尽管差异无统计学意义。还探讨了HGFs之间可能存在的协同效应(SE)。总体而言,在所研究的13例分选病例中有9例观察到协同生长,并且在CD34-或CD34+原始细胞部分中均可见此效应。对这些细胞完整表型特征进行分析后发现,根据CD15和HLA-DR抗原表达显示出SE的细胞部分更不成熟。我们可以得出结论,在白血病造血中,CD34抗原表达与正常造血中的意义不同,因为克隆形成细胞不限于CD34+急性髓系白血病(AML)原始细胞部分。此外,我们的研究表明,AML患者中观察到的对HGFs的异质性反应可能与免疫表型不同的原始细胞亚群的存在有关。
