Immunological Balance Is Associated with Clinical Outcome after Autologous Hematopoietic Stem Cell Transplantation in Type 1 Diabetes.

Kelen Cristina Ribeiro Malmegrim ,Lucas C M Arruda,Bart O Roep,Fabiano Pieroni,Daniela A Moraes,Renato Cunha,Richard K Burt,Luiza Guilherme,Joana R F Abreu,Carlos Eduardo Barra Couri ,Milton César Foss ,Júlio César Voltarelli ,Gislane Lelis Vilela De Oliveira ,Dimas Tadeu Covas ,Paulo César Rodrigues Palma ,Juliana Bernardes Elias Dias ,Nathália Paula Franco Santos ,Ana Beatriz Pereira Lima Stracieri ,Gabriela Trentin Scortegagna ,Belinda Pinto Simões ,Thalita Cristina De Mello Costa ,Maria Carolina De Oliveira

doi:10.3389/fimmu.2017.00167

Abstract

Autologous hematopoietic stem cell transplantation (AHSCT) increases C-peptide levels and induces insulin independence in patients with type 1 diabetes. This study aimed to investigate how clinical outcomes may associate with the immunological status, especially concerning the balance between immunoregulation and autoreactivity. Twenty-one type 1 diabetes patients were monitored after AHSCT and assessed every 6 months for duration of insulin independence, C-peptide levels, frequencies of islet-specific autoreactive CD8+ T cells (CTL), regulatory lymphocyte subsets, thymic function, and T-cell repertoire diversity. In median follow-up of 78 (range 15–106) months, all patients became insulin-independent, resuming insulin after median of 43 (range 6–100) months. Patients were retrospectively divided into short- or prolonged-remission groups, according to duration of insulin independence. For the entire follow-up, CD3+CD4+ T-cell numbers remained lower than baseline in both groups, whereas CD3+CD8+ T-cell levels did not change, resulting in a CD4/CD8 ratio inversion. Memory CTL comprehended most of T cells detected on long-term follow-up of patients after AHSCT. B cells reconstituted to baseline levels at 2–3 months post-AHSCT in both patient groups. In the prolonged-remission-group, baseline islet-specific T-cell autoreactivity persisted after transplantation, but regulatory T cell counts increased. Patients with lower frequencies of autoreactive islet-specific T cells remained insulin-free longer and presented greater C-peptide levels than those with lower frequencies of these cells. Therefore, immune monitoring identified a subgroup of patients with superior clinical outcome of AHSCT. Our study shows that improved immunoregulation may balance autoreactivity endorsing better metabolic outcomes in patients with lower frequencies of islet-specific T cells. Development of new strategies of AHSCT is necessary to increase frequency and function of T and B regulatory cells and decrease efficiently autoreactive islet-specific T and B memory cells in type 1 diabetes patients undergoing transplantation.

Highlights

Type 1 diabetes (T1D) results from T cell-mediated autoimmune destruction of β-cells from pancreatic islets, leading to insulin deficiency and hyperglycemia [1, 2]
These four patients did not experience any period of insulin freedom after Autologous hematopoietic stem cell transplantation (AHSCT)
Most patients in this study became insulin free for 3.5 years after transplantation and presented significant increments of C-peptide levels. This is different from the natural history of T1D and seems consonant with the hypothesis that a broad immunosuppressive approach could satisfactory control autoimmunity in diabetes [19, 20]

Summary

Introduction

Type 1 diabetes (T1D) results from T cell-mediated autoimmune destruction of β-cells from pancreatic islets, leading to insulin deficiency and hyperglycemia [1, 2]. Most studies showed little influence on β-cell function, at most keeping C-peptide levels stable while patients were under temporary immunosuppressive effects [4,5,6,7,8,9,10,11,12,13,14,15,16]. In these studies, no discontinuation of exogenous insulin injections was reported during 1–2 years follow-up. 21 out of 25 transplanted patients became insulin free after the procedure [19, 20]

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