Durable and controlled depletion of neutrophils in mice

Neutrophils are an essential part of the innate immune system. To study their importance, experimental studies often aim to deplete these cells, generally by injecting anti-Ly6G or anti-Gr1 antibodies. However, these approaches are only partially effective, transient or lack specificity. Here we report that neutrophils remaining after anti-Ly6G treatment are newly derived from the bone marrow, instead of depletion escapees. Mechanistically, newly generated, circulating neutrophils have lower Ly6G membrane expression, and consequently reduced targets for anti-Ly6G-mediated depletion. To overcome this limitation, we develop a double antibody-based depletion strategy that enhances neutrophil elimination by anti-Ly6G treatment. This approach achieves specific, durable and controlled reduction of neutrophils in vivo, and may be suitable for studying neutrophil function in experimental models.

Increased Myeloid Cell Production and Lung Bacterial Clearance in Mice Exposed to Cigarette Smoke

Alessandra Piersigilli

Pneumonia is a leading cause of hospitalization in patients with chronic obstructive pulmonary disease (COPD). Although most patients with COPD are smokers, the effects of cigarette smoke exposure on clearance of lung bacterial pathogens and on immune and inflammatory responses are incompletely defined. Here, clearance of Streptococcus pneumoniae and Pseudomonas aeruginosa and associated immune responses were examined in mice exposed to cigarette smoke or after smoking cessation. Mice exposed to cigarette smoke for 6 weeks or 4 months demonstrated decreased lung bacterial burden compared with air-exposed mice when infected 16 to 24 hours after exposure. When infection was performed after smoke cessation, bacterial clearance kinetics of mice previously exposed to smoke reversed to levels comparable to those of control mice, suggesting that the observed defects were not dependent on adaptive immunological memory to bacterial determinants found in smoke. Comparing cytokine levels and myeloid cell production before infection in mice exposed to cigarette smoke with mice never exposed or after smoke cessation revealed that reduced bacterial burden was most strongly associated with higher levels of IL-1 beta and granulocyte-macrophage colony-stimulating factor in the lungs and with increased neutrophil reserve and monocyte turnover in the bone marrow. Using Serpinb1a-deficient mice with reduced neutrophil numbers and treatment with granulocyte colony-stimulating factor showed that increased neutrophil numbers contribute only in part to the effect of smoke on infection. Our findings indicate that cigarette smoke induces a temporary and reversible increase in clearance of lung pathogens, which correlates with local inflammation and increased myeloid cell output from the bone marrow.

Amer Thoracic Soc2016

Neutrophils and Snail Orchestrate the Establishment of a Pro-tumor Microenvironment in Lung Cancer

Gael Luis Boivin, Julien Robert Rémi Faget, Miguel Garcia, Svenja Johanna Groeneveld, Nicolas Jean Philippe Guex, Etienne Meylan, Alessandra Piersigilli, Loïc Steiner, Ioannis Xenarios, Nadine Zangger

Understanding the immune compartment of tumors facilitates the development of revolutionary new therapies. We used a Kras(G12D)-driven mouse model of lung cancer to establish an immune signature and identified a contribution of Gr1 + neutrophils to disease progression. Depletion experiments showed that Gr1 + cells (1) favor tumor growth, (2) reduce T cell homing and prevent successful antiPD1 immunotherapy, and (3) alter angiogenesis, leading to hypoxia and sustained Snail expression in lung cancer cells. In turn, Snail accelerated disease progression and increased intratumoral Cxcl2 secretion and neutrophil infiltration. Cxcl2 was produced mainly by neutrophils themselves in response to a factor secreted by Snail-expressing tumor cells. We therefore propose a vicious cycle encompassing neutrophils and Snail to maintain a deleterious tumor microenvironment.

Cell Press2017

Investigation of transcriptional partners and genes downstream of Foxn1

Zineb Bekkali

The thymus is the second fundamental organ of the immune system after the bone marrow; it is the essential for T cell maturation and repertoire selection. The function of the thymus critically depends on the thymic epithelium, which is structured in two distinct regions: The cortex and the medulla. The knowledge about molecular mechanisms involved in thymus development is limited. However, some evidences suggest that the Hox, Pax, Six, Eya, Gcm2, FGFs and Foxn1 are key players in thymus organogenesis. Foxn1 is essential for thymic epithelial cell development but its exact role is still unknown. The null mutation in the transcription factor Foxn1 generates the nude phenotype of athymia and hairlessness. The aim of our laboratory is to better understand thymus development and specially focuses on the Foxn1 function. The aim of this project is then to investigate target genes and transcription partners of Foxn1 as a transcriptional factor. As a transcription factor, Foxn1 protein should be able to bind with DNA but should also interact with other proteins such as cofactors in order to activate its target genes. At present, the transcriptional partners of Foxn1 are completely unknown in the literature and the proteinprotein interaction databases. The experimental approach proposed here is the standard method for identification of unknown transcriptional partners: Immunoprecipitation (IP) followed by a mass spectrometry analysis. The list of protein candidates can then be validated by Western blotting. We identified the right antibodies to use for this procedure and optimised protocols for the IP. We also performed a mass spectrometry analysis that was not conclusive, however, the platform is now established to complete this analysis. Only little is known about genes up- or down-stream Foxn1. Some genes such as FgfR2IIIb, DLL4 and CCL25 are believed to be up-regulated by Foxn1. Our laboratory has generated a revertible hypomorphic allele of Foxn1 and have used this to obtain a series of six allelic combinations at Foxn1. These mice, expressing different levels of Foxn1, are a very useful tool in order to investigate target genes of Foxn1. In particular, we wish to investigate whether different Foxn1 targets are activated at different Foxn1 levels. 6 To reach this objective, the proposed approach is the comparison of gene expression profiles of thymic epithelial and mesenchymal cells of the allelic series at two different time points E13.5 and E15.5 using a Solexa tool called SAGE (Serial Analysis of Gene Expression). As preliminary analysis before the global gene expression analysis, we have determined expression profiles of several genes across the allelic series by quantitative PCR. Our findings suggest that DLL4, CCL25, FgfR2IIIb, FGF10 and possible Pax1 are direct or indirect targets of Foxn1 activated at different levels of Foxn1. DLL4 and CCL25 seem to be involved in lymphocyte attraction and maturation. FgfR2IIIb appears to be important for thymic epithelium differentiation and development by increasing the sensitivity of epithelial cells to FGF10 signalling. Finally, Pax1 is possibly required downstream of Foxn1 for terminal differentiation of cortical thymic epithelial cells

2009

Investigation of transcriptional partners and genes downstream of Foxn1

Zineb Bekkali

2009