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CD40L modulates transcriptional signatures of neutrophils in the bone marrow associated with development and trafficking
Tábata Takahashi França, Ashraf Al-Sbiei, Ghada Bashir, Yassir Awad Mohamed, Ranieri Coelho Salgado, Lucila Akune Barreiros, Sarah Maria da Silva Napoleão, Cristina Worm Weber, Janaíra Fernandes Severo Ferreira, Carolina Sanchez Aranda, Carolina Prando, Mayra B. de Barros Dorna, Igor Jurisica, Maria J. Fernandez-Cabezudo, Hans D. Ochs, Antonio Condino-Neto, Basel K. Al-Ramadi, Otavio Cabral-Marques
Tábata Takahashi França, Ashraf Al-Sbiei, Ghada Bashir, Yassir Awad Mohamed, Ranieri Coelho Salgado, Lucila Akune Barreiros, Sarah Maria da Silva Napoleão, Cristina Worm Weber, Janaíra Fernandes Severo Ferreira, Carolina Sanchez Aranda, Carolina Prando, Mayra B. de Barros Dorna, Igor Jurisica, Maria J. Fernandez-Cabezudo, Hans D. Ochs, Antonio Condino-Neto, Basel K. Al-Ramadi, Otavio Cabral-Marques
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Resource and Technical Advance Cell biology Immunology

CD40L modulates transcriptional signatures of neutrophils in the bone marrow associated with development and trafficking

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Abstract

Neutrophils are produced in the BM in a process called granulopoiesis, in which progenitor cells sequentially develop into mature neutrophils. During the developmental process, which is finely regulated by distinct transcription factors, neutrophils acquire the ability to exit the BM, properly distribute throughout the body, and migrate to infection sites. Previous studies have demonstrated that CD40 ligand (CD40L) influences hematopoiesis and granulopoiesis. Here, we investigate the effect of CD40L on neutrophil development and trafficking by performing functional and transcriptome analyses. We found that CD40L signaling plays an essential role in the early stages of neutrophil generation and development in the BM. Moreover, CD40L modulates transcriptional signatures, indicating that this molecule enables neutrophils to traffic throughout the body and to migrate in response to inflammatory signals. Thus, our study provides insights into the complex relationships between CD40L signaling and granulopoiesis, and it suggests a potentially novel and nonredundant role of CD40L signaling in neutrophil development and function.

Authors

Tábata Takahashi França, Ashraf Al-Sbiei, Ghada Bashir, Yassir Awad Mohamed, Ranieri Coelho Salgado, Lucila Akune Barreiros, Sarah Maria da Silva Napoleão, Cristina Worm Weber, Janaíra Fernandes Severo Ferreira, Carolina Sanchez Aranda, Carolina Prando, Mayra B. de Barros Dorna, Igor Jurisica, Maria J. Fernandez-Cabezudo, Hans D. Ochs, Antonio Condino-Neto, Basel K. Al-Ramadi, Otavio Cabral-Marques

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Figure 8

Neutrophils from patients with CD40L deficiency show impaired migration.

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Neutrophils from patients with CD40L deficiency show impaired migration....
(A) Representative figure of gating strategy used to quantify migrated neutrophils (n = 7). (B) Neutrophils from patients with CD40L deficiency and healthy individuals (healthy control) were incubated with PBS, fMLP (20 nM), IL-8 (10 nM), or C5a (25 nM). Spontaneous migration (PBS) of healthy individuals was normalized to 100%, and the other conditions were compared with the normalized value to assess the relative migration number (expressed in %) (n = 7 [P1, P2, and P3 evaluated more than once]; C5a: n = 5). (C) Gating strategy and histograms showing the pattern of expression of FPR1, CXCR2, and C5aR receptors in CD66b+ neutrophils from patients with CD40L deficiency (colored) and healthy individuals (gray, dotted line). (D) Expression of FPR1, CXCR2, and C5aR receptors expressed in log2 obtained from median fluorescence intensity (MFI) values. n = 4. *P < 0.05 (Mann-Whitney U test).

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