Abstract
Simple SummaryHodgkin lymphoma (HL) is composed of many reactive and only a few cancer cells, so-called Hodgkin and Reed-Sternberg (HRS) or lymphocyte predominant (LP) cells. Due to the scarcity of these cells, it was difficult to perform high-throughput molecular investigations on them for a long time. With the help of recently developed methods, it is now possible to analyze their genomes. This review summarizes the genetic alterations found in HRS and LP cells that impact immune evasion, proliferation and circumvention of programmed cell death in HL. Understanding these underlying molecular mechanisms is essential, as they may be of prognostic and predictive value and help to improve the therapy especially for patients with recurrent or treatment-resistant disease.Background: Hodgkin lymphoma (HL) is predominantly composed of reactive, non-neoplastic cells surrounding scarcely distributed tumor cells, that is, so-called Hodgkin and Reed-Sternberg (HRS) or lymphocyte predominant (LP) cells. This scarcity impeded the analysis of the tumor cell genomes for a long time, but recently developed methods (especially laser capture microdissection, flow cytometry/fluorescence-activated cell sorting) facilitated molecular investigation, elucidating the pathophysiological principles of “Hodgkin lymphomagenesis”. Methods: We reviewed the relevant literature of the last three decades focusing on the genomic landscape of classic and nodular lymphocyte predominant HL (NLPHL) and summarized molecular cornerstones. Results: Firstly, the malignant cells of HL evade the immune system by altered expression of PDL1/2, B2M and MHC class I and II due to various genetic alterations. Secondly, tumor growth is promoted by permanently activated JAK/STAT signaling due to pervasive mutations of multiple genes involved in the pathway. Thirdly, apoptosis of neoplastic cells is prevented by alterations of NF-κB compounds and the PI3K/AKT/mTOR axis. Additionally, Epstein-Barr virus infection can simultaneously activate JAK/STAT and NF-κB, similarly leading to enhanced survival and evasion of apoptosis. Finally, epigenetic phenomena such as promoter hypermethylation lead to the downregulation of B-lineage-specific, tumor-suppressor and immune regulation genes. Conclusion: The blueprint of HL genomics has been laid, paving the way for future investigations into its complex pathophysiology.
Highlights
Searching and Finding the Needle in the HaystackHodgkin lymphoma (HL) is unique in many aspects
In classic HL (cHL), almost all cell lines derive from refractory and relapsing cases, by no means reflecting the great majority of clinical courses [2]
In concordance with this study, our group was able to show a lack of SMAD1 expression due to hypermethylation of its promoter region in lymphocyte predominant (LP) and Hodgkin and Reed-Sternberg (HRS) cells of almost all studied clinical cases (14/14 nodular lymphocyte predominant HL (NLPHL) cases, 100% and 138/143 cHL cases, 97%)
Summary
Hodgkin lymphoma (HL) is unique in many aspects. In contrast to many other malignant tumors, HL escapes immunologic control but uses and recruits the immune system for its purposes, which leads to a significant and heterogeneous tumor microenvironment. In 2018, our group developed a novel fluorescence-activated cell sorting (FACS)-based enrichment technique for the isolation of HRS cells out of formalin-fixed and paraffin-embedded (FFPE) archival tissues [7] This involves DNA enrichment followed by whole-genome amplification and the application of a customized lymphoma panel assay of 68 genes [10]. The enrichment of tens of thousands of tumor cells is possible without potential laser radiationinduced DNA damage, the preservation of sufficient tissue antigenicity and cytometric recognition of specific signals remain obstacles in FFPE [7,11] Another promising and elegant approach is the analysis of circulating tumor DNA (ctDNA) of patients with cHL as reported by Spina et al [12] and most recently by Desch et al for pediatric HL patients [13].
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