Type IV pilus retraction enables sustained bacteremia and plays a key role in the outcome of meningococcal sepsis in a humanized mouse model

Neisseria meningitidis (the meningococcus) remains a major cause of bacterial meningitis and fatal sepsis. This commensal bacterium of the human nasopharynx can cause invasive diseases when it leaves its niche and reaches the bloodstream. Blood-borne meningococci have the ability to adhere to human endothelial cells and rapidly colonize microvessels. This crucial step enables dissemination into tissues and promotes deregulated inflammation and coagulation, leading to extensive necrotic purpura in the most severe cases. Adhesion to blood vessels relies on type IV pili (TFP). These long filamentous structures are highly dynamic as they can rapidly elongate and retract by the antagonistic action of two ATPases, PilF and PilT. However, the consequences of TFP dynamics on the pathophysiology and the outcome of meningococcal sepsis in vivo have been poorly studied. Here, we show that human graft microvessels are replicative niches for meningococci, that seed the bloodstream and promote sustained bacteremia and lethality in a humanized mouse model. Intriguingly, although pilus-retraction deficient N. meningitidis strain (ΔpilT) efficiently colonizes human graft tissue, this mutant did not promote sustained bacteremia nor induce mouse lethality. This effect was not due to a decreased inflammatory response, nor defects in bacterial clearance by the innate immune system. Rather, TFP-retraction was necessary to promote the release of TFP-dependent contacts between bacteria and, in turn, the detachment from colonized microvessels. The resulting sustained bacteremia was directly correlated with lethality. Altogether, these results demonstrate that pilus retraction plays a key role in the occurrence and outcome of meningococcal sepsis by supporting sustained bacteremia. These findings open new perspectives on the role of circulating bacteria in the pathological alterations leading to lethal sepsis.

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Evidence from a humanized mouse model of androgenetic alopecia that platelet‐rich plasma (PRP) stimulates hair regrowth, hair shaft diameter and vellus‐to‐terminal hair reconversion in vivo

British Journal of Dermatology ◽

10.1111/bjd.20084 ◽

2021 ◽

Author(s):

R. Laufer Britva ◽

A. Keren ◽

A. Ginzburg ◽

Y. Ullmann ◽

R. Paus ◽

...

Keyword(s):

Mouse Model ◽

Platelet Rich Plasma ◽

Hair Shaft ◽

Androgenetic Alopecia ◽

Humanized Mouse ◽

Humanized Mouse Model ◽

Terminal Hair ◽

Hair Regrowth ◽

Shaft Diameter

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P06.07 In vivo studies of immunomodulatory a-CTLA-4 antibody in a humanized mouse model

Journal for ImmunoTherapy of Cancer ◽

10.1136/jitc-2021-itoc8.41 ◽

2021 ◽

Vol 9 (Suppl 1) ◽

pp. A22.1-A22

Author(s):

C Reitinger ◽

F Nimmerjahn

Keyword(s):

Immune System ◽

Mouse Model ◽

Cancer Immunotherapy ◽

Model Systems ◽

Checkpoint Control ◽

Human Immune System ◽

Humanized Mouse ◽

Humanized Mouse Model ◽

Human Immune

BackgroundRecent findings in cancer immunotherapy have reinforced the hypothesis that the immune system is able to control most cancers. Immunomodulatory antibodies can enhance immune responses, having the potential to generate anti-cancer immunity.1–4Materials and MethodsMost current studies addressing this question are performed in murine mouse model systems or use in vitro culture systems, which do not reflect the human in vivo situation, potentially leading to results that cannot be fully translated into human cancer therapy. Therefore, it is necessary to establish a new mouse model, which allows the study of cancer immunotherapy in the context of a human immune system. We focused on the establishment of a humanized mouse model, in which different immunomodulatory antibodies can be tested in the presence of a human immune system.ResultsFirst experiments concerning the suitability to test immunomodulatory antibodies in the humanized mouse model, revealed that effects of checkpoint-control antibody a-CTLA-4 were similar to the effects seen in patients of clinical studies. To analyse the anti-tumor activities of immunomodulatory antibodies in vivo we are establishing a human melanoma-like tumor model in humanized mice.ConclusionsThis enables us to test the efficacy of immunomodulatory agonistic antibodies (such as CP-870,893) and checkpoint control antibodies (such as anti-CTLA-4) in eliminating a melanoma-like tumor. Furthermore, parameters like tumor infiltrating human cells und cytokine/chemokine production can be analysed.ReferencesSchuster M, Nechansky A, Loibner H. Cancer immunotherapy. Biotechnol J 2006;1:138–147.Mellman I, Coukos G, Dranoff G. Cancer immunotherapy comes of age. Nature rev 2011;480:480–489.Finn OJ. Immuno-oncology: understanding the function and dysfunction of the immune system in cancer. Annals of Oncology 2012;23:vii6–vii9.Langer LF, Clay TM, Morse MA. Update on anti-CTLA-4 in clinical trials. Expert Opin Biol Ther 2007;8:1245–1256.Disclosure InformationC. Reitinger: None. F. Nimmerjahn: None.

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In Vivo Gene Delivery into hCD34+ Cells in a Humanized Mouse Model

Methods in Molecular Biology - Viral Vectors for Gene Therapy ◽

10.1007/978-1-61779-095-9_15 ◽

2011 ◽

pp. 367-390 ◽

Cited By ~ 12

Author(s):

Cecilia Frecha ◽

Floriane Fusil ◽

François-Loïc Cosset ◽

Els Verhoeyen

Keyword(s):

Gene Delivery ◽

Mouse Model ◽

Humanized Mouse ◽

Humanized Mouse Model ◽

In Vivo Gene Delivery

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A novel humanized mouse model to study the function of human cutaneous memory T cells in vivo in human skin

Scientific Reports ◽

10.1038/s41598-020-67430-7 ◽

2020 ◽

Vol 10 (1) ◽

Cited By ~ 2

Author(s):

Maria M. Klicznik ◽

Ariane Benedetti ◽

Laura M. Gail ◽

Suraj R. Varkhande ◽

Raimund Holly ◽

...

Keyword(s):

T Cells ◽

Mouse Model ◽

Human Skin ◽

Memory T Cells ◽

Humanized Mouse ◽

Humanized Mouse Model

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Abstract 5465: Role of CYP2A13 in NNK bioactivation and lung tumorigenesis:In vivostudies using a CYP2A13-humanized mouse model

10.1158/1538-7445.am2012-5465 ◽

2012 ◽

Author(s):

Vandana Megaraj ◽

Xin Zhou ◽

Zhihua Liu ◽

Fang Xie ◽

Jaime D'Agostino ◽

...

Keyword(s):

Mouse Model ◽

Humanized Mouse ◽

Humanized Mouse Model

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In Vivo Anti-MicroRNA Treatment in a Humanized Mouse Model for Allograft Vasculopathy

The Journal of Heart and Lung Transplantation ◽

10.1016/j.healun.2017.01.1277 ◽

2017 ◽

Vol 36 (4) ◽

pp. S446

Author(s):

M. Huibers ◽

L. Qin ◽

G. Li ◽

J. Renes ◽

C. Venema ◽

...

Keyword(s):

Mouse Model ◽

Humanized Mouse ◽

Humanized Mouse Model ◽

Allograft Vasculopathy

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Human anti-CAIX antibodies mediate immune cell inhibition of renal cell carcinoma in vitro and in a humanized mouse model in vivo

Molecular Cancer ◽

10.1186/s12943-015-0384-3 ◽

2015 ◽

Vol 14 (1) ◽

Cited By ~ 23

Author(s):

De-Kuan Chang ◽

Raymond J. Moniz ◽

Zhongyao Xu ◽

Jiusong Sun ◽

Sabina Signoretti ◽

...

Keyword(s):

Renal Cell Carcinoma ◽

Mouse Model ◽

Cell Carcinoma ◽

Renal Cell ◽

Immune Cell ◽

Humanized Mouse ◽

Humanized Mouse Model ◽

Cell Inhibition

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Immune Activation and the Role of TLRs and TLR Agonists in the Pathogenesis of HIV-1 Infection in the Humanized Mouse Model

The Journal of Infectious Diseases ◽

10.1093/infdis/jit402 ◽

2013 ◽

Vol 208 (suppl_2) ◽

pp. S145-S149 ◽

Cited By ~ 5

Author(s):

J. Judy Chang ◽

Marcus Altfeld

Keyword(s):

Mouse Model ◽

Immune Activation ◽

Humanized Mouse ◽

Humanized Mouse Model ◽

Tlr Agonists ◽

Hiv 1

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Evaluation of 4-Amino 2-Anilinoquinazolines against Plasmodium and Other Apicomplexan Parasites In Vitro and in a P. falciparum Humanized NOD-scid IL2Rγnull Mouse Model of Malaria

Antimicrobial Agents and Chemotherapy ◽

10.1128/aac.01804-18 ◽

2018 ◽

Vol 63 (3) ◽

Cited By ~ 1

Author(s):

Paul R. Gilson ◽

William Nguyen ◽

William A. Poole ◽

Jose E. Teixeira ◽

Jennifer K. Thompson ◽

...

Keyword(s):

Mouse Model ◽

Babesia Bovis ◽

Parasite Line ◽

Humanized Mouse ◽

Humanized Mouse Model ◽

Content Type ◽

Apicomplexan Parasites ◽

Micromolar Range

ABSTRACT A series of 4-amino 2-anilinoquinazolines optimized for activity against the most lethal malaria parasite of humans, Plasmodium falciparum, was evaluated for activity against other human Plasmodium parasites and related apicomplexans that infect humans and animals. Four of the most promising compounds from the 4-amino 2-anilinoquinazoline series were equally as effective against the asexual blood stages of the zoonotic P. knowlesi, suggesting that they could also be effective against the closely related P. vivax, another important human pathogen. The 2-anilinoquinazoline compounds were also potent against an array of P. falciparum parasites resistant to clinically available antimalarial compounds, although slightly less so than against the drug-sensitive 3D7 parasite line. The apicomplexan parasites Toxoplasma gondii, Babesia bovis, and Cryptosporidium parvum were less sensitive to the 2-anilinoquinazoline series with a 50% effective concentration generally in the low micromolar range, suggesting that the yet to be discovered target of these compounds is absent or highly divergent in non-Plasmodium parasites. The 2-anilinoquinazoline compounds act as rapidly as chloroquine in vitro and when tested in rodents displayed a half-life that contributed to the compound’s capacity to clear P. falciparum blood stages in a humanized mouse model. At a dose of 50 mg/kg of body weight, adverse effects to the humanized mice were noted, and evaluation against a panel of experimental high-risk off targets indicated some potential off-target activity. Further optimization of the 2-anilinoquinazoline antimalarial class will concentrate on improving in vivo efficacy and addressing adverse risk.

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