Non-permissive human conventional CD1c+ dendritic cells enable trans-infection of human primary renal tubular epithelial cells and protect BK polyomavirus from neutralization.

Mathieu Sikorski,Steven Nedellec,Philippe Hulin,Flora Coulon,Régis Josien,Alexandra Garcia,Antoine Touzé,Julien Burlaud-Gaillard,Pauline Gaboriaud,Karine Renaudin,Matthieu Giraud,Céline Bressollette-Bodin,Cécile Peltier,Joëlle Véziers,Cécile Braudeau,Julien Branchereau,Christine Kandel-Aznar,Franck Halary,Dorian Mcilroy

doi:10.1371/journal.ppat.1009042

Abstract

The BK polyomavirus (BKPyV) is a ubiquitous human virus that persists in the renourinary epithelium. Immunosuppression can lead to BKPyV reactivation in the first year post-transplantation in kidney transplant recipients (KTRs) and hematopoietic stem cell transplant recipients. In KTRs, persistent DNAemia has been correlated to the occurrence of polyomavirus-associated nephropathy (PVAN) that can lead to graft loss if not properly controlled. Based on recent observations that conventional dendritic cells (cDCs) specifically infiltrate PVAN lesions, we hypothesized that those cells could play a role in BKPyV infection. We first demonstrated that monocyte-derived dendritic cells (MDDCs), an in vitro model for mDCs, captured BKPyV particles through an unconventional GRAF-1 endocytic pathway. Neither BKPyV particles nor BKPyV-infected cells were shown to activate MDDCs. Endocytosed virions were efficiently transmitted to permissive cells and protected from the antibody-mediated neutralization. Finally, we demonstrated that freshly isolated CD1c+ mDCs from the blood and kidney parenchyma behaved similarly to MDDCs thus extending our results to cells of clinical relevance. This study sheds light on a potential unprecedented CD1c+ mDC involvement in the BKPyV infection as a promoter of viral spreading.

Highlights

The BK polyomavirus (BKPyV) is a small non-enveloped DNA virus
Various studies reported a specific influx of myeloid dendritic cells in the renal tissue of kidney-transplant patients who were diagnosed with a BKPyV nephropathy
We showed that myeloid dendritic cells (mDCs) are unable to sense BKPyV particles or BKPyV-infected dying cells as a danger signal, supporting the view that other DC subsets might act as the true antigen presenting cells that promote the adaptive immune response against BKPyV infection

Summary

Introduction

The BK polyomavirus (BKPyV) is a small non-enveloped DNA virus. Its icosahedral capsid is mainly composed of the major capsid protein VP1[1,2,3]. Asymptomatic primary infection mostly occurs during childhood[6,7] followed by a persistent infection in the renourinary epithelium[8]. Evidence of BKPyV reactivation was reported in kidney and hematopoietic stem cell allografts [9,10,11,12], it has been well established that BKPyV, reactivating in KTRs, is mainly of donor origin[13,14,15,16,17]. Persistent BKPyV-DNAemia above 104 DNA copies/ml has been correlated to PVAN (overall 1–5% of KTRs)(18–20). BKPyV remains a significant cause of kidney graft failure[11,18]

Methods

Results

Discussion

Conclusion