Spatially resolved T cell receptor diversity mapping uncovers variability of the cancer immune microenvironment

Magoulopoulou, Anastasia; Chatzinikolaou, Maria; Metousis, Andreas; Hu, Taobo; Yu, Hui; Zerdes, Ioannis; Wang, Kang; Foukakis, Theodoros; Long, Mengping; Leandersson, Karin; Micke, Patrick; Strell, Carina; Nilsson, Mats

Spatially resolved T cell receptor diversity mapping uncovers variability of the cancer immune microenvironment

Mark

Magoulopoulou, Anastasia ; Chatzinikolaou, Maria ; Metousis, Andreas ; Hu, Taobo ; Yu, Hui ; Zerdes, Ioannis ; Wang, Kang ; Foukakis, Theodoros ; Long, Mengping and Leandersson, Karin ^LU

, et al. (2026) In EBioMedicine 127.

Abstract: Background: T cell receptor (TCR) binding properties have been related to a wide range of pathological conditions, including infections, autoimmunity and cancer. Characterising the TCR repertoire is of great biomedical interest but it has been challenging due to its high structural diversity. Methods: In situ sequencing (ISS) is a suitable technique for spatial cell typing and linking gene patterns directly to specific histopathological features of large biopsy areas. We applied ISS through the commercial Xenium platform, with the addition of a custom panel specifically designed for TCR gene detection. Based on the IMGT database, we selected unique target sequences for TCR genes encoding the constant, variable and joining TCR chains.... (More); Background: T cell receptor (TCR) binding properties have been related to a wide range of pathological conditions, including infections, autoimmunity and cancer. Characterising the TCR repertoire is of great biomedical interest but it has been challenging due to its high structural diversity. Methods: In situ sequencing (ISS) is a suitable technique for spatial cell typing and linking gene patterns directly to specific histopathological features of large biopsy areas. We applied ISS through the commercial Xenium platform, with the addition of a custom panel specifically designed for TCR gene detection. Based on the IMGT database, we selected unique target sequences for TCR genes encoding the constant, variable and joining TCR chains. Additionally, we developed an analysis pipeline for the assignment of putative clonotypes based on simultaneous expression of alpha and beta variable TCR chains (TCRVβ/Vα pairs) at the single-cell level. Findings: Our approach captured specific immune cell distributions in relation to the individual sample clonality, as well as regional dominance of certain TCRVβ/Vα pairs in surgical non-small cell lung cancer (NSCLC) specimens and matching lymph node samples. Furthermore, we were able to study the spatiotemporal evolution of TCR repertoire on longitudinal FFPE biopsies from patients with breast cancer, during neoadjuvant treatment. Interpretation: This study highlights the implementation of target-based spatially resolved transcriptomics for the spatial characterisation of TCRVβ/Vα pairs at the single-cell level, without the need for prior sequencing. Our approach allows for spatial immune characterisation of diagnostic tissue samples with emphasis on T cell biology and accompanying T cell diversity. Funding: This study was supported from Cancerfonden (CAN 2021/1726), Swedish Research Council (Dnr: 2019-01238), U-CAN and the Trond Mohn Foundation.
(Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/c785409f-8049-44c4-8f72-75f196def573

author

Magoulopoulou, Anastasia ; Chatzinikolaou, Maria ; Metousis, Andreas ; Hu, Taobo ; Yu, Hui ; Zerdes, Ioannis ; Wang, Kang ; Foukakis, Theodoros ; Long, Mengping and Leandersson, Karin ^LU

, et al. (More)

Magoulopoulou, Anastasia ; Chatzinikolaou, Maria ; Metousis, Andreas ; Hu, Taobo ; Yu, Hui ; Zerdes, Ioannis ; Wang, Kang ; Foukakis, Theodoros ; Long, Mengping ; Leandersson, Karin ^LU

; Micke, Patrick ; Strell, Carina and Nilsson, Mats (Less)

organization

publishing date

2026-05

type

Contribution to journal

publication status

published

subject

Cell and Molecular Biology

keywords

(ISS), (NSCLC), (SRT), (TCR), Breast cancer, In situ sequencing, Non-small cell lung cancer, Spatially resolved transcriptomics, T cell receptor, TCR diversity

in

EBioMedicine

volume

127

article number

106264

publisher

Elsevier

external identifiers

pmid:42034048
scopus:105036843929

ISSN

2352-3964

DOI

10.1016/j.ebiom.2026.106264

language

English

LU publication?

yes

id

c785409f-8049-44c4-8f72-75f196def573

date added to LUP

2026-05-19 15:04:21

date last changed

2026-06-02 16:06:15

@article{c785409f-8049-44c4-8f72-75f196def573,
  abstract     = {{<p>Background: T cell receptor (TCR) binding properties have been related to a wide range of pathological conditions, including infections, autoimmunity and cancer. Characterising the TCR repertoire is of great biomedical interest but it has been challenging due to its high structural diversity. Methods: In situ sequencing (ISS) is a suitable technique for spatial cell typing and linking gene patterns directly to specific histopathological features of large biopsy areas. We applied ISS through the commercial Xenium platform, with the addition of a custom panel specifically designed for TCR gene detection. Based on the IMGT database, we selected unique target sequences for TCR genes encoding the constant, variable and joining TCR chains. Additionally, we developed an analysis pipeline for the assignment of putative clonotypes based on simultaneous expression of alpha and beta variable TCR chains (TCRVβ/Vα pairs) at the single-cell level. Findings: Our approach captured specific immune cell distributions in relation to the individual sample clonality, as well as regional dominance of certain TCRVβ/Vα pairs in surgical non-small cell lung cancer (NSCLC) specimens and matching lymph node samples. Furthermore, we were able to study the spatiotemporal evolution of TCR repertoire on longitudinal FFPE biopsies from patients with breast cancer, during neoadjuvant treatment. Interpretation: This study highlights the implementation of target-based spatially resolved transcriptomics for the spatial characterisation of TCRVβ/Vα pairs at the single-cell level, without the need for prior sequencing. Our approach allows for spatial immune characterisation of diagnostic tissue samples with emphasis on T cell biology and accompanying T cell diversity. Funding: This study was supported from Cancerfonden (CAN 2021/1726), Swedish Research Council (Dnr: 2019-01238), U-CAN and the Trond Mohn Foundation.</p>}},
  author       = {{Magoulopoulou, Anastasia and Chatzinikolaou, Maria and Metousis, Andreas and Hu, Taobo and Yu, Hui and Zerdes, Ioannis and Wang, Kang and Foukakis, Theodoros and Long, Mengping and Leandersson, Karin and Micke, Patrick and Strell, Carina and Nilsson, Mats}},
  issn         = {{2352-3964}},
  keywords     = {{(ISS); (NSCLC); (SRT); (TCR); Breast cancer; In situ sequencing; Non-small cell lung cancer; Spatially resolved transcriptomics; T cell receptor; TCR diversity}},
  language     = {{eng}},
  publisher    = {{Elsevier}},
  series       = {{EBioMedicine}},
  title        = {{Spatially resolved T cell receptor diversity mapping uncovers variability of the cancer immune microenvironment}},
  url          = {{http://dx.doi.org/10.1016/j.ebiom.2026.106264}},
  doi          = {{10.1016/j.ebiom.2026.106264}},
  volume       = {{127}},
  year         = {{2026}},
}

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Spatially resolved T cell receptor diversity mapping uncovers variability of the cancer immune microenvironment