Chronic myeloid leukemia patients in prolonged remission following interferon-α monotherapy have distinct cytokine and oligoclonal lymphocyte profile.

Chronic myeloid leukemia patients in prolonged remission following interferon-α monotherapy have distinct cytokine and oligoclonal lymphocyte profile.

Before the era of tyrosine kinase inhibitors (TKIs), interferon-alpha (IFN-α) was the treatment of choice in chronic myeloid leukemia (CML). Curiously, some IFN-α treated patients were able to discontinue therapy without disease progression. The aim of this project was to study the immunomodulatory...

Full description

Bibliographic Details
Main Authors: Anna Kreutzman, Peter Rohon, Edgar Faber, Karel Indrak, Vesa Juvonen, Veli Kairisto, Jaroslava Voglová, Marjatta Sinisalo, Emília Flochová, Jukka Vakkila, Petteri Arstila, Kimmo Porkka, Satu Mustjoki
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2011-01-01
Series:PLoS ONE
Online Access:https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/21857985/pdf/?tool=EBI
id doaj-6dd371f4b6b64bb396523e3f23e118ab
record_format Article
spelling doaj-6dd371f4b6b64bb396523e3f23e118ab2021-03-04T01:40:31ZengPublic Library of Science (PLoS)PLoS ONE1932-62032011-01-0168e2302210.1371/journal.pone.0023022Chronic myeloid leukemia patients in prolonged remission following interferon-α monotherapy have distinct cytokine and oligoclonal lymphocyte profile.Anna KreutzmanPeter RohonEdgar FaberKarel IndrakVesa JuvonenVeli KairistoJaroslava VoglováMarjatta SinisaloEmília FlochováJukka VakkilaPetteri ArstilaKimmo PorkkaSatu MustjokiBefore the era of tyrosine kinase inhibitors (TKIs), interferon-alpha (IFN-α) was the treatment of choice in chronic myeloid leukemia (CML). Curiously, some IFN-α treated patients were able to discontinue therapy without disease progression. The aim of this project was to study the immunomodulatory effects of IFN-α in CML patients in prolonged remission and isolate biological markers predicting response. Due to rarity of patients on IFN-α monotherapy, a relatively small cohort of patients still on treatment (IFN-ON, n = 10, median therapy duration 11.8 years) or had discontinued IFN-α therapy but remained in remission for >2 years (IFN-OFF, n = 9) were studied. The lymphocyte immunophenotype was analyzed with a comprehensive flow cytometry panel and plasma cytokine levels were measured with multiplex bead-based assay. In addition, the clonality status of different lymphocyte subpopulations was analyzed by TCR γ/δ rearrangement assay. Median NK-cell absolute number and proportion from lymphocytes in blood was higher in IFN-OFF patients as compared to IFN-ON patients or controls (0.42, 0.19, 0.21×10(9)/L; 26%, 12%, 11%, respectively, p<0.001). The proportion of CD8+ T-cells was significantly increased in both patient groups and a larger proportion of T-cells expressed CD45RO. Most (95%) patients had significant numbers of oligoclonal lymphocytes characterized by T-cell receptor γ/δ rearrangements. Strikingly, in the majority of patients (79%) a distinct clonal Vγ9 gene rearrangement was observed residing in γδ(+) T-cell population. Similar unique clonality pattern was not observed in TKI treated CML patients. Plasma eotaxin and MCP-1 cytokines were significantly increased in IFN-OFF patients. Despite the limited number of patients, our data indicates that IFN-α treated CML patients in remission have increased numbers of NK-cells and clonal γδ(+) T-cells and a unique plasma cytokine profile. These factors may relate to anti-leukemic effects of IFN-α in this specific group of patients and account for prolonged therapy responses even after drug discontinuation.https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/21857985/pdf/?tool=EBI
collection DOAJ
language English
format Article
sources DOAJ
author Anna Kreutzman
Peter Rohon
Edgar Faber
Karel Indrak
Vesa Juvonen
Veli Kairisto
Jaroslava Voglová
Marjatta Sinisalo
Emília Flochová
Jukka Vakkila
Petteri Arstila
Kimmo Porkka
Satu Mustjoki
spellingShingle Anna Kreutzman
Peter Rohon
Edgar Faber
Karel Indrak
Vesa Juvonen
Veli Kairisto
Jaroslava Voglová
Marjatta Sinisalo
Emília Flochová
Jukka Vakkila
Petteri Arstila
Kimmo Porkka
Satu Mustjoki
Chronic myeloid leukemia patients in prolonged remission following interferon-α monotherapy have distinct cytokine and oligoclonal lymphocyte profile.
PLoS ONE
author_facet Anna Kreutzman
Peter Rohon
Edgar Faber
Karel Indrak
Vesa Juvonen
Veli Kairisto
Jaroslava Voglová
Marjatta Sinisalo
Emília Flochová
Jukka Vakkila
Petteri Arstila
Kimmo Porkka
Satu Mustjoki
author_sort Anna Kreutzman
title Chronic myeloid leukemia patients in prolonged remission following interferon-α monotherapy have distinct cytokine and oligoclonal lymphocyte profile.
title_short Chronic myeloid leukemia patients in prolonged remission following interferon-α monotherapy have distinct cytokine and oligoclonal lymphocyte profile.
title_full Chronic myeloid leukemia patients in prolonged remission following interferon-α monotherapy have distinct cytokine and oligoclonal lymphocyte profile.
title_fullStr Chronic myeloid leukemia patients in prolonged remission following interferon-α monotherapy have distinct cytokine and oligoclonal lymphocyte profile.
title_full_unstemmed Chronic myeloid leukemia patients in prolonged remission following interferon-α monotherapy have distinct cytokine and oligoclonal lymphocyte profile.
title_sort chronic myeloid leukemia patients in prolonged remission following interferon-α monotherapy have distinct cytokine and oligoclonal lymphocyte profile.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2011-01-01
description Before the era of tyrosine kinase inhibitors (TKIs), interferon-alpha (IFN-α) was the treatment of choice in chronic myeloid leukemia (CML). Curiously, some IFN-α treated patients were able to discontinue therapy without disease progression. The aim of this project was to study the immunomodulatory effects of IFN-α in CML patients in prolonged remission and isolate biological markers predicting response. Due to rarity of patients on IFN-α monotherapy, a relatively small cohort of patients still on treatment (IFN-ON, n = 10, median therapy duration 11.8 years) or had discontinued IFN-α therapy but remained in remission for >2 years (IFN-OFF, n = 9) were studied. The lymphocyte immunophenotype was analyzed with a comprehensive flow cytometry panel and plasma cytokine levels were measured with multiplex bead-based assay. In addition, the clonality status of different lymphocyte subpopulations was analyzed by TCR γ/δ rearrangement assay. Median NK-cell absolute number and proportion from lymphocytes in blood was higher in IFN-OFF patients as compared to IFN-ON patients or controls (0.42, 0.19, 0.21×10(9)/L; 26%, 12%, 11%, respectively, p<0.001). The proportion of CD8+ T-cells was significantly increased in both patient groups and a larger proportion of T-cells expressed CD45RO. Most (95%) patients had significant numbers of oligoclonal lymphocytes characterized by T-cell receptor γ/δ rearrangements. Strikingly, in the majority of patients (79%) a distinct clonal Vγ9 gene rearrangement was observed residing in γδ(+) T-cell population. Similar unique clonality pattern was not observed in TKI treated CML patients. Plasma eotaxin and MCP-1 cytokines were significantly increased in IFN-OFF patients. Despite the limited number of patients, our data indicates that IFN-α treated CML patients in remission have increased numbers of NK-cells and clonal γδ(+) T-cells and a unique plasma cytokine profile. These factors may relate to anti-leukemic effects of IFN-α in this specific group of patients and account for prolonged therapy responses even after drug discontinuation.
url https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/21857985/pdf/?tool=EBI
work_keys_str_mv AT annakreutzman chronicmyeloidleukemiapatientsinprolongedremissionfollowinginterferonamonotherapyhavedistinctcytokineandoligoclonallymphocyteprofile
AT peterrohon chronicmyeloidleukemiapatientsinprolongedremissionfollowinginterferonamonotherapyhavedistinctcytokineandoligoclonallymphocyteprofile
AT edgarfaber chronicmyeloidleukemiapatientsinprolongedremissionfollowinginterferonamonotherapyhavedistinctcytokineandoligoclonallymphocyteprofile
AT karelindrak chronicmyeloidleukemiapatientsinprolongedremissionfollowinginterferonamonotherapyhavedistinctcytokineandoligoclonallymphocyteprofile
AT vesajuvonen chronicmyeloidleukemiapatientsinprolongedremissionfollowinginterferonamonotherapyhavedistinctcytokineandoligoclonallymphocyteprofile
AT velikairisto chronicmyeloidleukemiapatientsinprolongedremissionfollowinginterferonamonotherapyhavedistinctcytokineandoligoclonallymphocyteprofile
AT jaroslavavoglova chronicmyeloidleukemiapatientsinprolongedremissionfollowinginterferonamonotherapyhavedistinctcytokineandoligoclonallymphocyteprofile
AT marjattasinisalo chronicmyeloidleukemiapatientsinprolongedremissionfollowinginterferonamonotherapyhavedistinctcytokineandoligoclonallymphocyteprofile
AT emiliaflochova chronicmyeloidleukemiapatientsinprolongedremissionfollowinginterferonamonotherapyhavedistinctcytokineandoligoclonallymphocyteprofile
AT jukkavakkila chronicmyeloidleukemiapatientsinprolongedremissionfollowinginterferonamonotherapyhavedistinctcytokineandoligoclonallymphocyteprofile
AT petteriarstila chronicmyeloidleukemiapatientsinprolongedremissionfollowinginterferonamonotherapyhavedistinctcytokineandoligoclonallymphocyteprofile
AT kimmoporkka chronicmyeloidleukemiapatientsinprolongedremissionfollowinginterferonamonotherapyhavedistinctcytokineandoligoclonallymphocyteprofile
AT satumustjoki chronicmyeloidleukemiapatientsinprolongedremissionfollowinginterferonamonotherapyhavedistinctcytokineandoligoclonallymphocyteprofile
_version_ 1714809366120497152

Similar Items