M-CSF attenuates severity of chronic GVHD after unrelated BMT

Kimura, Fumihiko; Sato, Ken; Akiyama, Hideki; Sao, Hiroshi; Okamoto, Shinichiro; Kobayashi, Naoki; Hara, Masamichi; Kawa, Keisei; Motoyoshi, Kazuo

doi:10.1038/bmt.2011.90

Cited by 9 publications

(8 citation statements)

References 19 publications

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“…Because M-CSF treatment reduces graft-versus-host disease in allogeneic HCT ( Hashimoto et al, 2011 ; Kimura et al, 2012 ), it will be important to determine whether it also has a protective effect against infection in this setting, as suggested by earlier retrospective clinical observations ( Nemunaitis et al, 1993 ). In this context, the influence of M-CSF treatment on graft-versus-leukemia effects and on residual malignant cells will also require further investigation.…”

Section: Resultsmentioning

confidence: 99%

M-CSF improves protection against bacterial and fungal infections after hematopoietic stem/progenitor cell transplantation

Kandalla

Sarrazin

Molawi

et al. 2016

Journal of Experimental Medicine

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Section: Resultsmentioning

confidence: 99%

M-CSF improves protection against bacterial and fungal infections after hematopoietic stem/progenitor cell transplantation

Kandalla

Sarrazin

Molawi

et al. 2016

Journal of Experimental Medicine

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“…The observed monocytosis highlights the importance of further studying the etiology of cGVHD, which might be related to chronic inflammation, as observed in autoimmune processes (40) or functional asplenia (41). Macrophage colony-stimulating factor (M-CSF) is a well-known inducer of monocytosis, and its administration to patients undergoing HSCT was shown to attenuate cGVHD (42), implicating that also, after HSCT, elevated M-CSF levels might drive monocyte expansion and alleviate cGVHD. Higher absolute monocyte counts were related with cGVHD, future cGVHD onset, higher NRM rate, as well as poor outcomes of allogeneic HSCT (43), and vice versa , monocyte recovery during the first year after HSCT may be associated with better outcome (44).…”

Section: Discussionmentioning

confidence: 99%

National Institutes of Health–Defined Chronic Graft-vs.-Host Disease in Pediatric Hematopoietic Stem Cell Transplantation Patients Correlates With Parameters of Long-Term Immune Reconstitution

et al. 2019

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Recent data revealed the importance of immune reconstitution (IR) for the evaluation of possible biomarkers in National Institutes of Health (NIH)–defined chronic graft-vs.-host disease (cGVHD) and its clinical aspects. In this large pediatric study ( n = 146), we have analyzed whether cellular and humoral parameters of IR in the long-term follow-up (FU) with a special emphasis on B-cell reconstitution correlate with NIH-defined cGVHD criteria. HYPOTHESIS: we were especially interested in whether meaningful cGVHD biomarkers could be defined in a large pediatric cohort. We here demonstrate for the first time in a highly homogenous pediatric patient cohort that both cGVHD ( n = 38) and its activity were associated with the perturbation of the B-cell compartment, including low frequencies of CD19 + CD27 + memory B-cells and increased frequencies of circulating CD19 + CD21 low B-cells, a well-known hyperactivated B-cell subset frequently found elevated in chronic infection and autoimmunity. Notably, resolution of cGVHD correlated with expansion of CD19 + CD27 + memory B-cells and normalization of CD19 + CD21 low B-cell frequencies. Moreover, we found that the severity of cGVHD had an impact on parameters of IR and that severe cGVHD was associated with increased CD19 + CD21 low B-cell frequencies. When comparing the clinical characteristics of the active and non-active cGVHD patients (in detail at time of analyses), we found a correlation between activity and a higher overall severity of cGVHD, which means that in the active cGVHD patient group were more patients with a higher disease burden of cGVHD—despite similar risk profiles for cGVHD. Our data also provide solid evidence that the time point of analysis regarding both hematopoietic stem cell transplantation (HSCT) FU and cGVHD disease activity may be of critical importance for the detailed investigation of pediatric cohorts. Finally, we have proven that the differences in risk factors and patterns of IR, with cGVHD as its main confounding factor, between malignant and non-malignant diseases, are important to be considered in future studies aiming at identification of novel biomarkers for cGVHD.

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“…We showed that IL‐34‐macrophages are more efficient to expand Tregs than CSF‐1‐macrophages and those Tregs are highly suppressive as they delay GVHD development in immune humanized NSG mice 25 . In human clinical trials, the protective role of CSF‐1 administration needs to be further investigated because some results showed improved recovery associated with less development of chronic GVHD 174,175 . However, another study indicated neither beneficial or deleterious role of CSF‐1 administration 176 .…”

Section: Overlapping and Non‐overlapping Functions Of Il‐34 And Csf‐1 In Diseasesmentioning

confidence: 96%

IL-34 and CSF-1, deciphering similarities and differences at steady state and in diseases

Freuchet

Salama

Remy

et al. 2021

Journal of Leukocyte Biology

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Although IL‐34 and CSF‐1 share actions as key mediators of monocytes/macrophages survival and differentiation, they also display differences that should be identified to better define their respective roles in health and diseases. IL‐34 displays low sequence homology with CSF‐1 but has a similar general structure and they both bind to a common receptor CSF‐1R, although binding and subsequent intracellular signaling shows differences. CSF‐1R expression has been until now mainly described at a steady state in monocytes/macrophages and myeloid dendritic cells, as well as in some cancers. IL‐34 has also 2 other receptors, protein‐tyrosine phosphatase zeta (PTPζ) and CD138 (Syndecan‐1), expressed in some epithelium, cells of the central nervous system (CNS), as well as in numerous cancers. While most, if not all, of CSF‐1 actions are mediated through monocyte/macrophages, IL‐34 has also other potential actions through PTPζ and CD138. Additionally, IL‐34 and CSF‐1 are produced by different cells in different tissues. This review describes and discusses similarities and differences between IL‐34 and CSF‐1 at steady state and in pathological situations and identifies possible ways to target IL‐34, CSF‐1, and its receptors.

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M-CSF attenuates severity of chronic GVHD after unrelated BMT

Cited by 9 publications

References 19 publications

M-CSF improves protection against bacterial and fungal infections after hematopoietic stem/progenitor cell transplantation

M-CSF improves protection against bacterial and fungal infections after hematopoietic stem/progenitor cell transplantation

National Institutes of Health–Defined Chronic Graft-vs.-Host Disease in Pediatric Hematopoietic Stem Cell Transplantation Patients Correlates With Parameters of Long-Term Immune Reconstitution

IL-34 and CSF-1, deciphering similarities and differences at steady state and in diseases

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