The Vitamin D Receptor-BIM Axis Overcomes Cisplatin Resistance in Head and Neck Cancer

Aya Khamis; Désirée Gül; Madita Wandrey; Qiang Lu; Shirley K Knauer; Christoph Reinhardt; Sebastian Strieth; Jan Hagemann; Roland H Stauber

doi:10.3390/cancers14205131

The Vitamin D Receptor-BIM Axis Overcomes Cisplatin Resistance in Head and Neck Cancer

Cancers (Basel). 2022 Oct 19;14(20):5131. doi: 10.3390/cancers14205131.

Authors

Aya Khamis^{1

2}, Désirée Gül¹, Madita Wandrey¹, Qiang Lu¹, Shirley K Knauer³, Christoph Reinhardt⁴, Sebastian Strieth⁵, Jan Hagemann¹, Roland H Stauber¹

Affiliations

¹ Department of Otorhinolaryngology Head and Neck Surgery, Molecular and Cellular Oncology, University Medical Center, 55131 Mainz, Germany.
² Oral Pathology Department, Faculty of Dentistry, Alexandria University, Alexandria 5372066, Egypt.
³ Centre for Medical Biotechnology (ZMB/CENIDE), Institute for Molecular Biology, University Duisburg-Essen, Universitätsstraße, 45117 Essen, Germany.
⁴ Center for Thrombosis and Hemostasis (CTH), University Medical Center Mainz, Langenbeckstrasse 1, 55131 Mainz, Germany.
⁵ Department of Otorhinolaryngology, University Medical Center Bonn, 53127 Bonn, Germany.

Abstract

Treatment success of head and neck squamous cell carcinoma (HNSCC) is often hindered by cisplatin resistance. As inherent and acquired therapy resistance counteracts improvement in long-term survival, novel multi-targeting strategies triggering cancer cell apoptosis are urgently required. Here, we identify the vitamin D receptor (VDR) as being significantly overexpressed in tumors of HNSCC patients (n = 604; p = 0.0059), correlating with tumor differentiation (p = 0.0002), HPV status (p = 0.00026), and perineural invasion (p = 0.0087). The VDR, a member of the nuclear receptor superfamily, is activated by its ligand vitamin D (VitD) and analogs, triggering multiple cellular responses. As we found that the VDR was also upregulated in our cisplatin-resistant HNSCC models, we investigated its effect on overcoming cisplatin resistance. We discovered that VitD/cisplatin combinations synergistically killed even cisplatin-resistant cells at clinically achievable levels. Similar results were obtained for the clinically used VitD analog Maxacalcitol. Moreover, VitD/cisplatin combinations inhibited tumor cell migration by E-cadherin upregulation. Signaling pathway analyses revealed that VitD co-treatments triggered cancer cell death by increasing the expression of the pro-apoptotic BCL-2 family protein BIM. BIM's pro-apoptotic activity in HNSCC cells was confirmed by ectopic overexpression studies. Importantly, BIM expression is positively associated with HNSCC patients' (n = 539) prognosis, as high expression correlated with improved survival (p = 0.0111), improved therapy response (p = 0.0026), and remission (p = 0.004). Collectively, by identifying, for the first time, the VDR/BIM axis, we here provide a molecular rationale for the reported anti-cancer activity of VitD/analogs in combination therapies. Our data also suggest its exploitation as a potential strategy to overcome cisplatin resistance in HNSCC and other malignancies by inducing additional pro-apoptotic pathways.

Keywords: HPV; calcitriol; combination therapy; nuclear receptors; platinum-based drugs; pro-apoptotic pathways; therapy resistance.

Abstract

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