AI Article Synopsis

  • High-throughput immune repertoire (IR) sequencing allows for an in-depth examination of B cell receptors (BCR) and T cell receptors (TCR), potentially improving the understanding and management of immune-related disorders.
  • The study used multiplex PCR to analyze BCR and TCR from bone marrow fluid (BMF) and peripheral blood (PB) of 17 patients, finding similar diversity in both sample types but notable differences in the distribution of monoclonal genes.
  • Results indicate that while PB samples can effectively monitor overall immune diversity, BMF samples remain essential for identifying specific monoclonal changes, aiding in clinical assessments and disease management strategies.

Article Abstract

High-throughput immune repertoire (IR) sequencing provides direct insight into the diversity of B cell receptor (BCR) and T cell receptor (TCR), with great potential to revolutionize the diagnosis, monitoring, and prevention of immune system-related disorders. In this study, multiplex PCR was applied to amplify the complementarity-determining regions of BCR and TCR, followed by comprehensive analysis by high-throughput sequencing. We compare the TCR (BCR) of bone marrow fluid (BMF) and peripheral blood (PB) samples from 17 patients in the Epstein-Barr and immunodeficiency groups, respectively. Our study shows that the diversity of the IR of blood samples is very similar to that of bone marrow samples statistically. However, the distributions of the monoclonal genes are significantly different in these 2 samples of most patients. This suggests that the BMFs can be replaced by the PB samples in diversity detection of IR to monitor the immune status of the body, while the detection of the BMFs is unreplaceable when the monoclonal change occurs. We used high-throughput sequencing to assess the TCR and BCR of the patients and provide a basis for the clinical analysis of PB and bone marrow samples and selection of disease diagnosis and monitoring methods.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11419465PMC
http://dx.doi.org/10.1097/MD.0000000000039501DOI Listing

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