HCA Data Explorer

Single-Cell Lymphocyte Heterogeneity in Advanced Cutaneous T-cell Lymphoma Skin Tumors

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Updated December 13, 2022

PurposeThe heterogeneity of tumor cells presents a major challenge to cancer diagnosis and therapy. Cutaneous T-cell lymphomas (CTCL) are a group of T lymphocyte malignancies that primarily affect skin. Lack of highly specific markers for malignant lymphocytes prevents early diagnosis, while only limited treatment options are available for patients with advanced stage CTCL. Droplet-based single-cell transcriptome analysis of CTCL skin biopsies opens avenues for dissecting patient-specific T lymphocyte heterogeneity, providing a basis for identifying specific markers for diagnosis and cure of CTCL.Experimental designSingle-cell RNA-sequencing was performed by Droplet-based sequencing (10X Genomics), focusing on 14,056 CD3+ lymphocytes (448 cells from normal and 13,608 cells from CTCL skin samples) from skin biopsies of 5 patients with advanced-stage CTCL and 4 healthy donors. Protein expression of identified genes was validated in advanced stage CTCL skin tumors by immunohistochemistry and confocal immunofluorescence microscopy.ResultsOur analysis revealed a large inter- and intratumor gene expression heterogeneity in the T lymphocyte subset, as well as a common gene expression signature in highly proliferating lymphocytes that was validated in multiple advanced-stage skin tumors. In addition, we established the immunologic state of reactive lymphocytes and found heterogeneity in effector and exhaustion programs across patient samples.ConclusionsSingle-cell analysis of CTCL skin tumor samples reveals patient-specific landscapes of malignant and reactive lymphocytes within the local microenvironment of each tumor, giving an unprecedented view of lymphocyte heterogeneity and identifying tumor-specific molecular signatures, with important implications for diagnosis and personalized disease treatment.

Patrizia FuschiottiDepartment of Medicine, Division of Rheumatology and Clinical Immunology, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania. paf23@pitt.edu.paf23@pitt.edu
Alyxzandria M Gaydosik1
Tracy Tabib1
Larisa J Geskin2
Claire-Audrey Bayan2
James F Conway3
Robert Lafyatis1
Patrizia Fuschiotti4
1Department of Medicine, Division of Rheumatology and Clinical Immunology, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania.
2Columbia University Medical Center, New York, New York.
3Department of Structural Biology, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania.
4Department of Medicine, Division of Rheumatology and Clinical Immunology, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania. paf23@pitt.edu.
Ami Day

To reference this project, please use the following link:

https://explore.data.humancellatlas.org/projects/990d251f-6dab-4a98-a2b6-6cfe7e4708b9
None
GEO Series Accessions:

Atlas

None

Analysis Portals

None

Project Label

TCellLymphomaHeterogeneity

Species

Homo sapiens

Sample Type

specimens

Anatomical Entity

skin of body

Organ Part

Unspecified

Selected Cell Types

Unspecified

Disease Status (Specimen)

2 disease statuses

Disease Status (Donor)

2 disease statuses

Development Stage

human adult stage

Library Construction Method

10X 3' v2

Nucleic Acid Source

single cell

Paired End

false

Analysis Protocol

analysis_protocol_raw

File Format

2 file formats

Cell Count Estimate

14.1k

Donor Count

9
csv.gz9 file(s)xlsx1 file(s)