Literature DB >> 23439310

Humanized mice, a new model to study the influence of drug treatment on neonatal sepsis.

Wolfgang Ernst1, Nicole Zimara, Frank Hanses, Daniela N Männel, Birgit Seelbach-Göbel, Anja K Wege.   

Abstract

Bacterial infection with group B Streptococcus (GBS) represents a prominent threat to neonates and fetuses in the Western world, causing severe organ damage and even death. To improve current therapeutic strategies and to investigate new approaches, an appropriate in vivo model to study the immune response of a human immune system is needed. Therefore, we introduced humanized mice as a new model for GBS-induced sepsis. Humanized mice feature deficiencies similar to those found in neonates, such as lower immunoglobulin levels and myeloid cell dysfunction. Due to the husbandry in specific-pathogen-free (SPF) facilities, the human immune cells in these mice also exhibit a naive phenotype which mimics the conditions in fetuses/neonates. Following infection, cytokine release and leukocyte trafficking from the bone marrow to the lymphoid organ (spleen) and into the peritoneum (site of infection) as well as bacterial spreading and clearance were traceable in the humanized mice. Furthermore, we investigated the effects of betamethasone and indomethacin treatment using this novel sepsis model. Although both drugs are commonly used in perinatal care, little is known about their effects on the neonatal immune system. Treatment of infected humanized mice not only induced the reduction of human leukocytes in the spleen but also increased the bacterial load in all analyzed organs, including the brain, which did not show infiltration of live GBS in untreated controls. These studies demonstrate the utility of the humanized mice as a new model to study an immature human immune response during bacterial infection and allow the investigation of side effects induced by various treatments.

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Year:  2013        PMID: 23439310      PMCID: PMC3647987          DOI: 10.1128/IAI.01235-12

Source DB:  PubMed          Journal:  Infect Immun        ISSN: 0019-9567            Impact factor:   3.441


  65 in total

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6.  Defective innate immunity predisposes murine neonates to poor sepsis outcome but is reversed by TLR agonists.

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Review 8.  Group B streptococcus and early-onset sepsis in the era of maternal prophylaxis.

Authors:  Joyce M Koenig; William J Keenan
Journal:  Pediatr Clin North Am       Date:  2009-06       Impact factor: 3.278

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Review 10.  Understanding the regulation of Group B Streptococcal virulence factors.

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  13 in total

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Journal:  Clin Microbiol Rev       Date:  2017-10       Impact factor: 26.132

2.  Mice engrafted with human hematopoietic stem cells support a human myeloid cell inflammatory response in vivo.

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3.  Co-transplantation of human hematopoietic stem cells and human breast cancer cells in NSG mice: a novel approach to generate tumor cell specific human antibodies.

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Journal:  MAbs       Date:  2014-05-08       Impact factor: 5.857

4.  Humanizing the mouse: in defense of murine models of critical illness.

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Review 5.  Humanized Mouse Models of Clinical Disease.

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Review 7.  Group B Streptococcal Maternal Colonization and Neonatal Disease: Molecular Mechanisms and Preventative Approaches.

Authors:  Kathryn A Patras; Victor Nizet
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9.  Anti-inflammatory Activity of MTL-CEBPA, a Small Activating RNA Drug, in LPS-Stimulated Monocytes and Humanized Mice.

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Journal:  Mol Ther       Date:  2019-02-26       Impact factor: 11.454

Review 10.  Potential Pitfalls of the Humanized Mice in Modeling Sepsis.

Authors:  Krzysztof Laudanski; Michael Stentz; Matthew DiMeglio; William Furey; Toby Steinberg; Arpit Patel
Journal:  Int J Inflam       Date:  2018-09-02
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