New therapies in onco-hematology and new infectious risk factors.

Ilaria Del Giudice, Robin Foà
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Abstract

The biologic, clinical and therapeutic setting is nowadays such that risk factors for infectious complications are constantly changing and progressively increasing in patients suffering from onco-hematologic conditions. In addition to situations that are well known or that are gradually being recognized related both to the underlying disease and to treatment, such as neutropenia, neutrophil dysfunction, mucosal damage, concomitant monocytopenia and lymphopenia, abnormalities within the host cellular and humoral compartments, impairments in cytokine networks, alterations in T lymphocytes/tumor interactions, crosstalks between neoplastic cells and accessory cells, etc, over the last few years we are witnessing important changes in the overall management of patients with hematologic malignancies. Historically, the categories at risk were represented by patients with acute leukemia and patients undergoing an allogeneic stem cell transplant. In both, the likelihood of eradicating the disease requires necessarily a myeloablative therapeutic strategy, complicated in the allografted patients by the risks of graft-versus-host disease (GvHD), the required immunosuppressive treatment and the recently documented role that cytokines may play in the development of acute GvHD. Considerable changes have occurred in recent years. From the identification of "new" diseases at risk (e.g. lymphomas occurring in HIV+ individuals), to the progressive and constant increase in allotransplant procedures, to the development of new transplant procedures (cord blood, matched-unrelated or mismatched donor transplant, mini-transplant, the administration of donor lymphocytes), to the development of new drugs that can induce immunosuppression, to the clinical use of certain monoclonal antibodies (MoAb), to the combined use of chemotherapy plus MoAb. These developments are associated with other general considerations. Within these: 1) the growing use of ablative therapies in diseases for which for many years the approach has been less aggressive or indeed conservative; 2) the progressive recognition of categories of patients with unfavorable prognosis for whom an aggressive approach is required; 3) the constant improvement in mean life expectancy and "biologic" age of patients; thus, the progressive changes in the definition of "old age". Taken together, this has led, on the one hand, to an increase in the categories of onco-hematologic patients at risk of infective complications and to a major focus on the immune compartment of the affected patients, and, on the other hand, to an overall broadening of the infective scenario.

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肿瘤血液学的新疗法和新的感染危险因素。
当今的生物学、临床和治疗环境使得感染并发症的危险因素不断变化,并且在患有血液肿瘤疾病的患者中逐渐增加。除了众所周知的或逐渐被认识到与潜在疾病和治疗相关的情况,如中性粒细胞减少症、中性粒细胞功能障碍、粘膜损伤、伴随的单核细胞减少症和淋巴细胞减少症、宿主细胞和体液区室的异常、细胞因子网络的损伤、T淋巴细胞/肿瘤相互作用的改变、肿瘤细胞和辅助细胞之间的相互作用等,在过去的几年中,我们目睹了血液恶性肿瘤患者总体管理的重要变化。从历史上看,有风险的类别是急性白血病患者和接受同种异体干细胞移植的患者。在这两种情况下,根除这种疾病的可能性都需要一种清除骨髓的治疗策略,在同种异体移植患者中,移植物抗宿主病(GvHD)的风险、所需的免疫抑制治疗以及最近记录的细胞因子可能在急性GvHD发展中发挥的作用使其复杂化。近年来发生了很大的变化。从发现有危险的"新"疾病(例如艾滋病毒阳性个体发生的淋巴瘤),到异体移植程序的逐步和不断增加,到发展新的移植程序(脐带血、不匹配或不匹配的供体移植、微型移植、供体淋巴细胞的管理),到开发可诱导免疫抑制的新药,到某些单克隆抗体的临床使用,化疗加摩押联合使用。这些发展与其他一般考虑有关。其中包括:1)消融治疗越来越多地用于多年来治疗方法不那么激进或实际上保守的疾病;2)逐步识别预后不良、需要积极治疗的患者类别;3)患者的平均预期寿命和“生物学”年龄不断提高;于是,“老年”的定义逐渐发生了变化。综上所述,这一方面导致了有感染并发症风险的肿瘤血液病患者类别的增加,并主要关注受影响患者的免疫室,另一方面导致了感染情况的全面扩大。
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