Author
Listed:
- Adam P. Jones
(The University of Manchester
University of Manchester)
- Michael J. Haley
(The University of Manchester
University of Manchester)
- Miriam H. Meadows
(The University of Manchester
University of Manchester)
- Grace E. Gregory
(University of Manchester
The University of Manchester)
- Cathal J. Hannan
(University of Manchester
Salford Royal Hospital NHS Foundation Trust)
- Ana K. Simmons
(The University of Manchester)
- Leoma D. Bere
(The University of Manchester
University of Manchester)
- Daniel G. Lewis
(University of Manchester
Salford Royal Hospital NHS Foundation Trust)
- Pedro Oliveira
(The Christie Hospital)
- Miriam J. Smith
(University of Manchester
The University of Manchester)
- Andrew T. King
(University of Manchester
Salford Royal Hospital NHS Foundation Trust)
- D. Gareth R. Evans
(University of Manchester
The University of Manchester)
- Pawel Paszek
(The University of Manchester
Polish Academy of Sciences)
- David Brough
(University of Manchester
The University of Manchester)
- Omar N. Pathmanaban
(University of Manchester
The University of Manchester
Salford Royal Hospital NHS Foundation Trust)
- Kevin N. Couper
(The University of Manchester
University of Manchester)
Abstract
NF2-related Schwannomatosis (NF2 SWN) is a rare disease characterised by the growth of multiple nervous system neoplasms, including bilateral vestibular schwannoma (VS). VS tumours are characterised by extensive leucocyte infiltration. However, the immunological landscape in VS and the spatial determinants within the tumour microenvironment that shape the trajectory of disease are presently unknown. In this study, to elucidate the complex immunological networks across VS, we performed imaging mass cytometry (IMC) on clinically annotated VS samples from NF2 SWN patients. We reveal the heterogeneity in neoplastic cell, myeloid cell and T cell populations that co-exist within VS, and that distinct myeloid cell and Schwann cell populations reside within varied spatial contextures across characteristic Antoni A and B histomorphic niches. Interestingly, T-cell populations co-localise with tumour-associated macrophages (TAMs) in Antoni A regions, seemingly limiting their ability to interact with tumorigenic Schwann cells. This spatial landscape is altered in Antoni B regions, where T-cell populations appear to interact with PD-L1+ Schwann cells. We also demonstrate that prior bevacizumab treatment (VEGF-A antagonist) preferentially reduces alternatively activated-like TAMs, whilst enhancing CD44 expression, in bevacizumab-treated tumours. Together, we describe niche-dependent modes of T-cell regulation in NF2 SWN VS, indicating the potential for microenvironment-altering therapies for VS.
Suggested Citation
Adam P. Jones & Michael J. Haley & Miriam H. Meadows & Grace E. Gregory & Cathal J. Hannan & Ana K. Simmons & Leoma D. Bere & Daniel G. Lewis & Pedro Oliveira & Miriam J. Smith & Andrew T. King & D. G, 2025.
"Spatial mapping of immune cell environments in NF2-related schwannomatosis vestibular schwannoma,"
Nature Communications, Nature, vol. 16(1), pages 1-18, December.
Handle:
RePEc:nat:natcom:v:16:y:2025:i:1:d:10.1038_s41467-025-57586-z
DOI: 10.1038/s41467-025-57586-z
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