Summary: | Ensaios clinicos tem demonstrado que a imunossupressao em altas doses (IAD) seguida de transplante autologo de celulas tronco hematopoeticas (TACTH) e capaz de suprimir a atividade inflamatoria em pacientes com doencas autoimunes (DAIs) e induzir remissoes clinicas prolongadas nesses pacientes, porem os mecanismos de acao do TACTH ainda nao estao bem esclarecidos. O racional dessa terapia baseia-se na eliminacao das celulas autorreativas pela IAD e na reconstituicao de um sistema imunologico novo e tolerante apos o transplante a partir dos precursores hematopoeticos. O objetivo deste trabalho foi avaliar a reconstituicao imunologica em pacientes com diabetes mellitus tipo 1 (DM1, N=21) e pacientes com esclerose multipla (EM, N=37) sequencialmente apos o TACTH, e correlacionar os dados imunologicos com a resposta clinica dos pacientes ao transplante. Os pacientes com EM e DM1 foram divididos em dois grupos com base na resposta clinica apos o transplante: respondedores (EM-R; N=22) e nao-respondedores (EM-NR; N=15); livres de insulina por periodo maior ou igual a 3 anos (DM13 anos; N=11) e livres de insulina por periodo menor que 3 anos (DM1<3 anos; n=10); e acompanhados clinica e imunofenotipicamente por seis anos. Em relacao ao periodo pre-transplante, todos os grupos de pacientes com DM1 e EM apresentaram: 1, diminuicao do numero absoluto de celulas T CD3+ praticamente em todos os periodos pos-transplante avaliados, indicando uma intensa linfopenia decorrente da IAD; 2, aumento acentuado do numero de linfocitos T CD8+ e a diminuicao dos linfocitos T CD4+, resultando na inversao da razao CD4:CD8 durante todo o seguimento pos-transplante avaliado; 3, aumento significativo no primeiro ano apos o transplante das subpopulacoes de celulas T CD8+ de memoria central CD27+CD45RO+ e memoria efetora CD27- CD45RO+; 4, normalizacao dos numeros de linfocitos T CD4+ e CD8+ naive CD27+CD45RO- somente cinco anos apos o transplante, enquanto o numero de celulas T CD4+CD45RA+CD31+ recem- emigrantes do timo manteve-se abaixo dos valores pre-transplante durante todo o periodo avaliado, demonstrando que durante os seis anos de seguimento apos a IAD/TACTH predominaram mecanismos timo-independentes de reconstituicao imunologica; 5, normalizacao dos numeros de linfocitos B CD19+ entre dois a tres meses pos-transplante. O grupo de pacientes com DM1 que obteve melhor resposta clinica apos o tratamento com IAD/TACTH (DM13anos) apresentou, em comparacao ao periodo pre-transplante, numero diminuido de celulas T CD3+ (linfopenia) em varios periodos pos-transplante, numero aumentado de celulas T CD8+CD28- supressoras no primeiro ano pos-transplante principalmente, numero diminuido de celulas T CD4+ de memoria efetora nos periodos 2 a 9 meses pos-transplante e numero aumentado de celulas T reguladoras CD4+CD25hiFOXP3+ pos-transplante. O grupo de pacientes com EM com melhor resposta clinica apos o tratamento com IAD/TACTH (EM-R) apresentou, em comparacao ao periodo pre-transplante, numero diminuido de celulas T CD3+ (linfopenia) em varios periodos pos-transplante e numeros aumentados de celulas T reguladoras CD4+CD25hiFOXP3+ e CD8+CD28- supressoras nos primeiros tres anos pos-transplante. Vale ressaltar que os pacientes com DM1 e EM que apresentaram melhor resposta clinica permaneceram linfopenicos por maiores periodos de tempo apos o transplante. Desse modo, esse estudo revelou que a resposta terapeutica dos pacientes com DM1 e EM ao TACTH depende de uma linfopenia persistente, alem do aumento de celulas T reguladoras e supressoras e diminuicao de celulas T CD4+ de memoria apos o transplante. === Clinical trials have shown that high-dose immunosuppression (HDI) followed by autologous hematopoietic stem cell transplantation (AHSCT) is able to suppress the inflammatory activity in patients with autoimmune diseases (AID) and induce prolonged clinical remissions in these patients, but the mechanisms of action of AHSCT are still not well understood. The rationale of this therapy is based on the elimination of autoreactive cells by HDI and on the reconstitution of a new tolerant immune system after transplantation from hematopoietic precursors. The aim of this study was to evaluate the immune reconstitution in patients with type 1 diabetes mellitus (T1D, N=21) and patients with multiple sclerosis (MS, N=37) sequentially after the AHSCT, and correlate the immunological data with the clinical response of these patients to the transplant. Patients with MS and T1D were divided into two groups based on clinical response following transplantation: response (MS-R, N=22) and non-response (MS-NR, N=15); insulin-free for a period longer or equal to 3 years (T1D3 years, n=11) and insulin-free for less than 3 years (T1D<3 years, n=10); and accompanied clinical and immunophenotypically by six years. Regarding the pre-transplant period, all groups of patients with T1D and MS showed: 1, decreased absolute number of CD3+ T cells in virtually all post-transplant periods evaluated, indicating an intense lymphopenia resulting from HDI; 2, sharp increase in the number of CD8+ T lymphocytes and decreased CD4+ T lymphocytes, resulting in inversion of CD4:CD8 ratio throughout the follow-up post-transplant evaluation; 3, a significant increase, in the first year after transplantation, of CD8+ T central memory CD27+CD45RO+ and effector memory CD27-CD45O+ cell subpopulations; 4, normalization of CD4+ and CD8+ T naive CD27+CD45RO- lymphocytes numbers only five years after transplantation, whereas the number of CD4+CD45RA+CD31+ T cells newly emigrants from the thymus remained below the values pre- transplant during the study period, showing that during the six years of follow-up after the HDI/AHSCT mechanisms thymus-independent immune reconstitution were predominant; 5, normalization of CD19+ B lymphocytes numbers in two to three months post-transplant. The group of patients with DM1 that had the best clinical response after treatment with IAD/AHSCT (T1D 3years) showed, in comparison with the pre-transplant period, decreased number of CD3+ T cells (lymphopenia) at various times after transplantation, increased CD8+CD28- suppressor T cells numbers in the first year post-transplant, decreased number of CD4+ effector memory in periods of 2 and 9 months post-transplant and increased number of CD4+CD25hiFOXP3+ regulatory T cells after transplantation. The group of MS patients with better clinical response after treatment with IAD/AHSCT (MS-R) showed, in comparison to the pre-transplant period, decreased number of CD3+ T cells (lymphopenia) at various times after transplantation and increased numbers of CD4+CD25hiFOXP3+ regulatory Tcell and CD8+CD28- suppressor in the first three years post- transplant. It is noteworthy that patients with T1D and MS which showed better clinical response remained lymphopenic for longer periods of time after transplantation. Thus, this study revealed that the therapeutic response of patients with T1D and MS depend on a AHSCT to persistent lymphopenia, and increased regulatory and suppressor T cells and decreased number of CD4+ effector memory after transplantation.
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