Hadzidimitriou Anastasia, Stamatopoulos Kostas, Belessi Chrysoula, Lalayianni Chrysavgi, Stavroyianni Niki, Smilevska Tatjana, Hatzi Katerina, Laoutaris Nikolaos, Anagnostopoulos Achilles, Kollia Panagoula, Fassas Athanasios
Hematology Department and Hematopoietic Cell Transplantation Unit, G. Papanicolaou Hospital, Thessalonik, Greece.
Haematologica. 2006 Jun;91(6):781-7.
The available data on the immunoglobulin gene (IG) repertoire in multiple myeloma (MM) derive mainly from heavy chains; considerably less is known about light chains. We assessed in parallel IGH and IGK/IGL rearrangements in 101 MM patients so as to gain insight into: (i) IG repertoires; (ii) antigen impact; (iii) the role of receptor editing.
Bone marrow aspirates were collected from all cases. IGHV-(D)-J and IGLV-J rearrangements were amplified by reverse transcriptase polymerase chain reaction (PCR). In all cases, IGKV-J rearrangements were analyzed in parallel on cDNA/genomic DNA. IGKV-KDE and IGKJ-C-INTRON-KDE were also amplified by DNA-PCR. RT-PCR products were directly sequenced.
IGHV3 genes predominated; the IGHV4-34 gene was used in only one case. Five IGKV and five IGLV genes accounted for the majority of in-frame, transcribed IGKV-J or IGLV-J rearrangements. Taking IGKV-J, IGKV-KDE and IGKJ-C-INTRON-KDE rearrangements together, biallelic IGK locus rearrangements were detected in 22/43 k-MM cases. In l-MM, 36/42 cases had at least one rearranged IGK allele; 8/19 IGKV-J rearrangements in l-MM were in-frame. All in-frame, transcribed IGH/IGK/IGL sequences were mutated; parallel heavy/light chain analysis demonstrated a comparable impact of somatic hypermutation.
Biases in IG repertoire did not seem disease-related but followed a similar pattern to that of the normal repertoire. The under-representation of the IGHV4-34 gene provides an explanation for the paucity of autoimmune phenomena in MM. Somatic mutation patterns indicate the complementary role of MM IGH/IGK/IGL sequences in antigen recognition. Finally, the frequent inactivation of productive IGKV-J joints by secondary rearrangements in MM suggests active receptor editing.
关于多发性骨髓瘤(MM)免疫球蛋白基因(IG)库的现有数据主要来自重链;而轻链方面的了解则少得多。我们对101例MM患者的IGH和IGK/IGL重排进行了平行评估,以深入了解:(i)IG库;(ii)抗原影响;(iii)受体编辑的作用。
收集所有病例的骨髓穿刺液。通过逆转录聚合酶链反应(PCR)扩增IGHV-(D)-J和IGLV-J重排。在所有病例中,对cDNA/基因组DNA同时进行IGKV-J重排分析。还通过DNA-PCR扩增IGKV-KDE和IGKJ-C-INTRON-KDE。RT-PCR产物直接测序。
IGHV3基因占主导;仅1例使用IGHV4-34基因。5个IGKV和5个IGLV基因占框内转录的IGKV-J或IGLV-J重排的大部分。将IGKV-J、IGKV-KDE和IGKJ-C-INTRON-KDE重排综合考虑,在22/43例κ-MM病例中检测到双等位基因IGK基因座重排。在λ-MM中,36/42例至少有一个重排的IGK等位基因;λ-MM中8/19例IGKV-J重排为框内重排。所有框内转录的IGH/IGK/IGL序列均发生突变;平行重链/轻链分析显示体细胞超突变的影响相当。
IG库中的偏差似乎与疾病无关,但遵循与正常库相似的模式。IGHV4-34基因的低表达解释了MM中自身免疫现象的缺乏。体细胞突变模式表明MM的IGH/IGK/IGL序列在抗原识别中起互补作用。最后,MM中通过二次重排导致有功能的IGKV-J接头频繁失活提示存在活跃的受体编辑。
