# Immune Cell-Specific and Isoform-Selective Regulation of CD44 in Pancreatic Ductal Adenocarcinoma Links Lymph Node Variant Loss and Exosomal CD44 to Clinical Outcome in Pancreatic Ductal Adenocarcinoma

**Authors:** Alara Karabiber, Yong Zhou, Anke Mittelstädt, Frederik Johannes Hansen, Melanie Litau, Isabelle Kuchenreuther, Johanne Mazurie, Finn Niklas Clausen, Sebastian Klöckner, Franziska Czubayko, Nadine Weisel, Bettina Klösch, Talida Andert-Veres, Stefanie Kröber, Susanne Merkel, Andreas R. R. Weiss, Maximilian Brunner, Christian Krautz, Robert Grützmann, Georg F. Weber, Paul David

PMC · DOI: 10.3390/cells15050411 · 2026-02-27

## TL;DR

This study explores how CD44, a cell surface protein, is regulated in immune cells and exosomes in pancreatic cancer, linking its variants to disease progression and treatment resistance.

## Contribution

The study reveals immune cell-specific and isoform-selective regulation of CD44 in pancreatic cancer, linking exosomal CD44 and variant isoform loss to clinical outcomes.

## Key findings

- CD44 variant isoforms v4–v10 are significantly reduced in PDAC lymph nodes and associated with metastasis and poor survival.
- Exosomal CD44 levels are reduced in PDAC but elevated in patients with metastasis and poor survival.
- High CD44 expression correlates with immune infiltration, checkpoint gene expression, and resistance to chemotherapy drugs like gemcitabine.

## Abstract

Pancreatic ductal adenocarcinoma (PDAC) is characterized by immune cell dysfunction and poor prognosis. CD44, a cell surface glycoprotein with multiple splice variants, has been implicated in tumor progression, but its compartment-specific roles in PDAC remain unclear. CD44 standard and variant isoform expression was analyzed in patient-derived lymph nodes (LNs) by quantitative PCR. Immune cell-specific CD44 expression was assessed by flow cytometry in LNs and peripheral blood. Soluble and exosome-associated CD44 (exo-CD44) were measured in plasma. Clinical associations and survival analyses were performed. Transcriptomic, immune infiltration, immune checkpoint, and drug sensitivity analyses were conducted using TCGA-PAAD and pharmacogenomic datasets. CD44 standard isoform expression was unchanged in PDAC LNs, whereas multiple CD44 variant isoforms (v4–v10) were significantly reduced and associated with metastatic disease and poor survival, particularly CD44v5, v6, v7, and v10. CD44 expression was enriched in CD45+ immune cells, with highest levels in CD4+ T cells in both LNs and blood. Soluble CD44 levels showed no clinical associations. In contrast, exo-CD44 levels were reduced overall in PDAC but increased in patients with distant metastasis, positive resection margins, systemic inflammation, and reduced survival. High CD44 expression was associated with advanced disease, immune cell infiltration, immune checkpoint gene expression, reduced sensitivity to gemcitabine, paclitaxel, rapamycin, and FMK, and distinct CTLA4/PD-L1 checkpoint profiles. CD44 exhibits compartment-specific regulation in PDAC, linking immune remodeling, exosome signaling, and therapeutic resistance to adverse clinical outcome.

## Linked entities

- **Genes:** CD44 (CD44 molecule (IN blood group)) [NCBI Gene 960]
- **Proteins:** CD44 (CD44 molecule (IN blood group)), CTLA4 (cytotoxic T-lymphocyte associated protein 4), CD274 (CD274 molecule)
- **Chemicals:** gemcitabine (PubChem CID 60750), paclitaxel (PubChem CID 36314), rapamycin (PubChem CID 5284616), FMK (PubChem CID 644243)
- **Diseases:** pancreatic ductal adenocarcinoma (MONDO:0005184), metastatic disease (MONDO:0024883)

## Full-text entities

- **Genes:** CD274 (CD274 molecule) [NCBI Gene 29126] {aka ADMIO5, B7-H, B7H1, PD-L1, PDCD1L1, PDCD1LG1}, PTPRC (protein tyrosine phosphatase receptor type C) [NCBI Gene 5788] {aka B220, CD45, CD45R, GP180, IMD105, L-CA}, CD4 (CD4 molecule) [NCBI Gene 920] {aka CD4mut, IMD79, Leu-3, OKT4D, T4}, CTLA4 (cytotoxic T-lymphocyte associated protein 4) [NCBI Gene 1493] {aka ALPS5, CD, CD152, CELIAC3, CTLA-4, GRD4}, CD44 (CD44 molecule (IN blood group)) [NCBI Gene 960] {aka CDW44, CSPG8, ECM-III, ECMR-III, H-CAM, HCELL}
- **Diseases:** metastasis (MESH:D009362), PDAC (MESH:D021441), inflammation (MESH:D007249), metastatic disease (MESH:D000092182), tumor (MESH:D009369)
- **Chemicals:** rapamycin (MESH:D020123), paclitaxel (MESH:D017239), FMK (-), gemcitabine (MESH:D000093542)
- **Species:** Homo sapiens (human, species) [taxon 9606]

## Figures

7 figures with captions in the complete paper: https://tomesphere.com/paper/PMC12984284/full.md

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Source: https://tomesphere.com/paper/PMC12984284