Progressive multifocal leukoencephalopathy (PML) is a rare viral infection of the central nervous system (CNS) occurring in immunocompromised patients. Recovery of JC virus (JCV) specific T cell immune responses is the only available therapeutic option. JCV may use immune checkpoint inhibitory pathways to evade immune responses. The aim of this project is to determine whether T cell expression of immune checkpoint molecules is correlated to antiviral T cell responses, control of JCV replication and PML outcome. Immune checkpoint blockade by reversing T cell exhaustion may represent a therapeutic perspective for PML.
PML is a devastating orphan disease of the CNS due to the reactivation of JCV in immunocompromised patients. Given the lack of drugs controlling JCV replication, initiation of antiretroviral therapy in HIV-infected patients or cessation of immunosuppressive therapies in others, and subsequent recovery of JCV-specific T cell immune responses remains to date the only available therapeutic option. Promoting antiviral immune responses may improve the control of viral replication and the outcome of this severe disease. Immune checkpoint molecules such as PD-1 are inhibitory receptors expressed on T cells that trigger inhibitory signaling pathways, limiting effector immune responses in cancer and chronic infections. Immune checkpoint inhibitory pathways implicated in evading immune responses may be at play in PML. Immune checkpoint blockade using monoclonal antibodies targeting PD-1, by reversing T cell exhaustion, has been suggested as a therapeutic perspective for PML. More insights in the dynamics of immune checkpoint molecules expressed by T cells in PML patients are needed to pave the way for a therapeutic study. The aim here is to determine whether T cell expression of a broad range of immune checkpoint molecules, and its dynamics, correlates with the generation of antiviral of immune responses, the control of JCV replication and PML outcome. To this end the investigators will recruit 15 PML patients from 4 teaching hospitals in the South West of France and assess at PML diagnosis and 1, 3 and 6 months after, the expression of immune checkpoint molecules on circulating T cells, ex vivo specific immune responses against a JCV peptide library, JC viral load in cerebrospinal fluid, blood and urine, and clinical and neuroradiological outcomes.
Study Type
INTERVENTIONAL
Allocation
NA
Purpose
BASIC_SCIENCE
Masking
NONE
Enrollment
22
Collection of blood (47 mL) and urine (5 mL) at PML diagnosis and 1, 3 and 6 months after, for analysis of immune checkpoint molecules expression, detection of antiviral immune responses and virological analyses.
Spinal tap for monitoring of JC viral load at PML diagnosis and 1, 3 and 6 months after, and collection of CSF (2 mL) for virological analyses.
Brain MRI at at PML diagnosis and 3 and 6 months after
Neurological evaluation at PML diagnosis and 1, 3 and 6 months after
CHU Bordeaux
Bordeaux, France
CHU Montpellier
Montpellier, France
CHU de TOULOUSE
Toulouse, France
Immune checkpoint molecules
Expression level of a broad panel of immune checkpoint molecules by T cells at PML diagnosis bu flow cytometry
Time frame: 1 month
Immune checkpoint molecules
Expression level of a broad panel of immune checkpoint molecules by T cells at PML diagnosis bu flow cytometry
Time frame: 3 months
Immune checkpoint molecules
Expression level of a broad panel of immune checkpoint molecules by T cells at PML diagnosis bu flow cytometry
Time frame: 6 months
JC viral load
JC viral load in cerebrospinal fluid, blood and urine by ultra-sensitive PCR at PML diagnosis
Time frame: 1 month
JC viral load
JC viral load in cerebrospinal fluid, blood and urine by ultra-sensitive PCR at PML diagnosis
Time frame: 3 months
JC viral load
JC viral load in cerebrospinal fluid, blood and urine by ultra-sensitive PCR at PML diagnosis
Time frame: 6 months
Detection of immune responses against a JCV peptide library
Detection of specific immune responses against a JCV peptide library at PML diagnosis by flow cytometry
Time frame: 1 month
Detection of immune responses against a JCV peptide library
Detection of specific immune responses against a JCV peptide library at PML diagnosis by flow cytometry
Time frame: 3 months
Detection of immune responses against a JCV peptide library
Detection of specific immune responses against a JCV peptide library at PML diagnosis by flow cytometry
Time frame: 6 months
Differential impact of immune checkpoint inhibition
Differential impact of immune checkpoint inhibition in vitro on detection of specific immune responses at PML diagnosis by flow cytometry
Time frame: 1 month, 3 months and 6 months
Clinical outcome with Performance status
Clinical outcome using validated scales such as Performance status at PML diagnosis
Time frame: 1 month, 3 months and 6 months
Clinical outcome with NIHSS
Clinical outcome using validated scales such as NIHSS (National Institute of Health Stroke Score) at PML diagnosis
Time frame: 1 month, 3 months and 6 months
Clinical outcome with Rankin
Clinical outcome using validated scales such as Rankin at PML diagnosis
Time frame: 1 month, 3 months and 6 months
Neuroradiological monitoring
Neuroradiological monitoring by brain MRI at PML diagnosis
Time frame: 3 months and 6 months
JC virus genotyping
JC virus genotyping in blood, cerebrospinal fluid (CSF) and urine by ultra-sensitive PCR at PML diagnosis
Time frame: 1 month, 3 months and 6 months
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