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利用 KIR 基因分型在移植医学中的实际考虑和工作流程。

Practical Considerations and Workflow in Utilizing KIR Genotyping in Transplantation Medicine.

机构信息

Department of Paediatrics, Yong Loo Lin School of Medicine, National University of Singapore, Singapore, Singapore.

National University Health System, Singapore, Singapore.

出版信息

Methods Mol Biol. 2022;2463:291-310. doi: 10.1007/978-1-0716-2160-8_20.

Abstract

This chapter is intended to serve as a practical guide for establishing a workflow using sequence-specific polymorphism PCR (SSP-PCR) for killer cell immunoglobulin-like receptor (KIR) genotyping in a clinical setting, especially in allogeneic hematopoietic stem cell transplantation (HSCT). As clinical evidence accumulates on the application of KIR and HLA genetics to guide donor selection in HSCT, there is an increasing need for KIR genotyping in clinical settings, and thus medical institutes may need to build this capability. Among the various KIR genotyping approaches now available, SSP-PCR methods are well-established and are the most cost-effective and will likely be the method of choice especially when expenses will be passed on to the patient. The protocol described in this chapter developed by Vilches et al. features small amplicon PCR and is suitable for KIR genotyping using FFPE-derived DNA as well as DNA extracted from blood samples. Setting up a laboratory workflow for in-house KIR genotyping is relatively straightforward; in this chapter, considerations for KIR genotyping to guide clinical decisions are discussed.In HSCT, a main objective of KIR genotyping is to apply the genetic analysis to predict donor and recipient combinations that have the most potential to produce NK cell alloresponses either through the missing-self mechanism or by action associated with activating KIR. The desired effects are reduction in acute GVHD and relapse rates and enhancement of overall survival. The information herein may also be useful to clinical laboratories considering the application of KIR genotyping in areas such as solid organ transplantation, NK cell-based treatment in other forms of cancer and autoimmune diseases, humanized antibody treatment, regenerative medicine, and reproductive medicine. Some background knowledge on KIR genetics will be necessary in managing a KIR genotyping platform. This chapter aims to address the main difficulties often encountered by physicians in understanding the KIR system, such as basic aspects of the nomenclature of KIR genes and haplotypes, genotypes, and determining presence/absence of KIR ligands in the patient and donor from the extensively diversified HLA class I allotypes. In describing the workflow, emphasis has been placed on the processes after genotype PCR and gel image acquisition: haplotype inference, generating B content scores, deduction of KIR ligands from HLA typing results, and the emerging algorithms for donor selection based on KIR and HLA genetics.

摘要

本章旨在为临床环境中使用序列特异性多态性聚合酶链反应(SSP-PCR)建立杀伤细胞免疫球蛋白样受体(KIR)基因分型工作流程提供实用指南,特别是在异基因造血干细胞移植(HSCT)中。随着 KIR 和 HLA 遗传学在 HSCT 中指导供者选择的临床证据不断积累,临床环境中对 KIR 基因分型的需求不断增加,因此医疗机构可能需要建立这种能力。在目前可用的各种 KIR 基因分型方法中,SSP-PCR 方法已经成熟,并且是最具成本效益的方法,尤其是当费用将转嫁给患者时。本章描述的由 Vilches 等人开发的协议具有小扩增子 PCR 的特点,适用于使用 FFPE 衍生 DNA 以及从血液样本中提取的 DNA 进行 KIR 基因分型。建立内部 KIR 基因分型的实验室工作流程相对简单;在本章中,讨论了指导临床决策的 KIR 基因分型的考虑因素。在 HSCT 中,KIR 基因分型的主要目标是应用遗传分析来预测供者和受者组合,这些组合最有可能通过缺失自我机制或与激活 KIR 相关的作用产生 NK 细胞同种异体反应。期望的效果是降低急性移植物抗宿主病和复发率,并提高总生存率。本文中的信息对于考虑将 KIR 基因分型应用于实体器官移植、NK 细胞在其他形式的癌症和自身免疫性疾病中的治疗、人源化抗体治疗、再生医学和生殖医学等领域的临床实验室也可能有用。在管理 KIR 基因分型平台时,需要一些关于 KIR 遗传学的背景知识。本章旨在解决医生在理解 KIR 系统时经常遇到的主要困难,例如 KIR 基因和单倍型的命名法、基因型以及从广泛多样化的 HLA Ⅰ类同种异型中确定患者和供者中 KIR 配体的存在/缺失等基本方面。在描述工作流程时,重点放在基因型 PCR 和凝胶图像采集后的过程上:单倍型推断、生成 B 含量评分、从 HLA 分型结果推断 KIR 配体以及基于 KIR 和 HLA 遗传学的供者选择新兴算法。

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