Tong A W, Zhang B Q, Mues G, Solano M, Hanson T, Stone M J
Cancer Immunology Research Laboratory, Charles A. Sammons Cancer Center, Baylor University Medical Center, Dallas, TX 75246.
Blood. 1994 Nov 1;84(9):3026-33.
Ligand binding of the B-cell lineage antigen CD40 enhances growth and interleukin-6 (IL-6) secretion in human B cells (the CD40/IL-6 loop). IL-6 has an autocrine and paracrine role in human multiple myeloma (MM) cell growth. With the use of the CD40 monoclonal antibody (MoAb) G28-5, we examined CD40 expression and the effect of CD40 binding on MM clonogenic colony (MCC) formation to characterize the IL-6/CD40 loop activity in MM. CD40 was expressed on plasmacytoid cells in 21 of 28 plasma cell dyscrasia (PCD) bone marrow (BM) biopsies tested (10 of 14 MM, 2 of 2 Waldenstrom's macroglobulinemia [WM], 2 of 2 plasma cell leukemia [PCL], 6 of 8 monoclonal gammopathy of undetermined significance [MGUS], and 1 of 2 primary amyloidosis [AL]). G28-5 binding increased MCCs by 35% to 150% in 11 of 17 CD40+ PCD BM cultures, but did not affect MCC formation in CD40- specimens or normal BM colony forming units (CFU-GEMM, CFU-GM, BFU-E). Responsive cultures originated from BM of patients with MM (2 of 5 cases tested), WM (2 of 2), PCL (2 of 2), and MGUS (5 of 6). CD40-responsiveness was not significantly inhibited by the presence of an anti-IL-6 MoAb (2 of 2 MGUS cultures tested), and did not correlate with the capacity to respond to IL-6 stimulation (n = 17, P > .05) or a detectable level of endogenous IL-6 (n = 15, P > .05). Additional studies were performed with PCD cell lines to characterize the interrelationship of CD40 activation and IL-6 production. Fifty percent to greater than 95% of cells from the RPMI 8226 and ARH77 lines expressed CD40, whereas 6% of U266 cells were CD40+. For RPMI 8226, ARH-77, and U266 cells, the increased MCC formation after anti-CD40 stimulation was not affected by the presence of an anti-IL-6 neutralizing MoAb and was not accompanied by detectable IL-6 secretion. There was no apparent increase in IL-6 mRNA transcription following G28-5 treatment of U266 or RPMI 8226 cells. Our observations indicate that CD40 is expressed in a subset of human myeloma cells present in various PCDs. Cell-line studies suggest that the CD40+ myeloma cell may regulate MM clonogenic colony formation without activating the IL-6 pathway.
B细胞谱系抗原CD40的配体结合可增强人B细胞的生长及白细胞介素-6(IL-6)分泌(CD40/IL-6环路)。IL-6在人多发性骨髓瘤(MM)细胞生长中具有自分泌和旁分泌作用。我们使用CD40单克隆抗体(MoAb)G28-5,检测了CD40表达以及CD40结合对MM克隆形成集落(MCC)形成的影响,以表征MM中的IL-6/CD40环路活性。在检测的28例浆细胞异常(PCD)骨髓(BM)活检组织中的21例中,浆细胞样细胞表达CD40(14例MM中的10例、2例瓦尔登斯特伦巨球蛋白血症[WM]中的2例、2例浆细胞白血病[PCL]中的2例、8例意义未明的单克隆丙种球蛋白病[MGUS]中的6例以及2例原发性淀粉样变性[AL]中的1例)。在17例CD40+ PCD BM培养物中的11例中,G28-5结合使MCC增加了35%至150%,但对CD-40标本或正常BM集落形成单位(CFU-GEMM、CFU-GM、BFU-E)的MCC形成没有影响。反应性培养物来源于MM患者(检测的5例中有2例)、WM(2例中的2例)、PCL(2例中的2例)和MGUS(6例中的5例)的BM。抗IL-6 MoAb的存在并未显著抑制CD40反应性(检测的2例MGUS培养物),且与对IL-6刺激的反应能力(n = 17,P > 0.05)或内源性IL-6的可检测水平(n = 15,P > 0.05)无关。我们使用PCD细胞系进行了额外研究,以表征CD40激活与IL-6产生之间的相互关系。来自RPMI 8226和ARH77细胞系的50%至超过95%的细胞表达CD40,而U266细胞的6%为CD40+。对于RPMI 8226、ARH-77和U266细胞,抗CD40刺激后MCC形成增加不受抗IL-6中和MoAb存在的影响,且未伴有可检测到的IL-6分泌。用G28-5处理U266或RPMI 8226细胞后,IL-6 mRNA转录没有明显增加。我们的观察结果表明,CD40在存在于各种PCD中的一部分人骨髓瘤细胞中表达。细胞系研究表明,CD40+骨髓瘤细胞可能在不激活IL-途径的情况下调节MM克隆形成集落的形成
