The human cationic host defense peptide LL-37 mediates contrasting effects on apoptotic pathways in different primary cells of the innate immune system

Barlow, Peter G.; Li, Yuexin; Wilkinson, Thomas S.; Bowdish, Dawn M. E.; Lau, YL; Cosseau, Céline; Haslett, Christopher; Simpson, A. John; Hancock, Robert E. W.; Davidson, Donald J.

doi:10.1189/jlb.1005560

Cited by 147 publications

(177 citation statements)

References 69 publications

(113 reference statements)

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“…Mononuclear cell layers were collected, washed twice in PBS, and the cells seeded at 1 3 10 6 cells/ml in RPMI 1640 with 10% heat-inactivated FCS, 2 mM L-glutamine, and 1 mM sodium pyruvate (all from Invitrogen), in a humidified incubator at 37˚C and 5% CO 2 . Neutrophils were isolated as previously described (10). Blood was prediluted in 2% (w/v) Dextran T-500 (Amersham Biosciences) in 0.9% saline and sedimented for 30 min at room temperature.…”

Section: Cell Isolation and Culturementioning

confidence: 99%

“…The microbicidal activity of peptides is due to their preferential interactions with prokaryotic membranes, leading to bacterial membrane disruption and/or targeting of intracellular bacterial molecules (5,6). The immunomodulatory activities of such peptides are extremely diverse and include stimulation of chemotaxis and chemokine production (7,8), promotion of leukocyte antimicrobial functions (9), regulation of neutrophil and epithelial cell apoptosis (10,11), regulation of dendritic cell differentiation and activation, stimulation of epithelial cell migration and wound healing, promotion of angiogenesis, and many others (reviewed in Refs. 12,13).…”

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confidence: 99%

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Synthetic Cationic Peptide IDR-1002 Provides Protection against Bacterial Infections through Chemokine Induction and Enhanced Leukocyte Recruitment

Nijnik

Madera

et al. 2010

The Journal of Immunology

182

224

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With the rapid rise in the incidence of multidrug resistant infections, there is substantial interest in host defense peptides as templates for production of new antimicrobial therapeutics. Natural peptides are multifunctional mediators of the innate immune response, with some direct antimicrobial activity and diverse immunomodulatory properties. We have previously developed an innate defense regulator (IDR) 1, with protective activity against bacterial infection mediated entirely through its effects on the immunity of the host, as a novel approach to anti-infective therapy. In this study, an immunomodulatory peptide IDR-1002 was selected from a library of bactenecin derivatives based on its substantially more potent ability to induce chemokines in human PBMCs. The enhanced chemokine induction activity of the peptide in vitro correlated with stronger protective activity in vivo in the Staphylococcus aureus-invasive infection model, with a >5-fold reduction in the protective dose in direct comparison with IDR-1. IDR-1002 also afforded protection against the Gram-negative bacterial pathogen Escherichia coli. Chemokine induction by IDR-1002 was found to be mediated through a Gi-coupled receptor and the PI3K, NF-κB, and MAPK signaling pathways. The protective activity of the peptide was associated with in vivo augmentation of chemokine production and recruitment of neutrophils and monocytes to the site of infection. These results highlight the importance of the chemokine induction activity of host defense peptides and demonstrate that the optimization of the ex vivo chemokine-induction properties of peptides is a promising method for the rational development of immunomodulatory IDR peptides with enhanced anti-infective activity.

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Section: Cell Isolation and Culturementioning

confidence: 99%

mentioning

confidence: 99%

Synthetic Cationic Peptide IDR-1002 Provides Protection against Bacterial Infections through Chemokine Induction and Enhanced Leukocyte Recruitment

Nijnik

Madera

et al. 2010

The Journal of Immunology

182

224

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“…P2X7R KO-derived macrophages do not release IL-1 in response to ATP, resulting on an attenuated acute inflammatory response (Labasi et al, 2002;Lister et al, 2007). Normal function of the P2X7R results in an optimal acute phase response that extends the life cycle of neutrophils (Barlow et al, 2006). An inefficient acute response can lead to an overwhelming chronic response: massive macrophage infiltration, abundant apoptotic and necrotic cells, and generalized tissue damage (Lister et al, 2007).…”

Section: Orthodontic Mechanotransduction and The Role Of The P2x7 Recmentioning

confidence: 99%

Orthodontic mechanotransduction and the role of the P2X7 receptor

Viecilli

Katona

Chen

et al. 2009

American Journal of Orthodontics and Dentofacial Orthopedics

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DEDICATIONTo my parents, who have supported my education. iv ACKNOWLEDGMENTSOne of the most important things I have learned during my PhD is the necessity of the existence of a working network of people that can help you achieve your goals. The more effectively this network functions, the higher the chance you will achieve the goals quickly.I would first like to thank my parents, who have unconditionally supported my decision to abandon a profitable private practice in Orthodontics, and return to humble student conditions while aiming for a full time academic career.I also thank my girlfriend Laura Kruter who has (almost always) been ok with my, some might say, not very sane ideas. Sometimes they do turn out fine, though (like this "PhD" one).I can hardly think of anyone else that could have complemented my work and ideas during this Program as well as Dr. Thomas Katona. While I was passionately conditioned to an idea, he was always rational and careful. While I was sometimes furious with a shortcoming, he was always temperate and humorous. When I ran into his office with some news about a project, he would always listen and almost never seem too busy to see me. While I was working and something went wrong, he would listen and wonder with me about the "whys" and "hows", instead of telling me what to do or express disappointment. He was even subject to some of my home culinary experiments. I was extremely fortunate to find someone that thought about science the same way I did, and that actually helped me with my project instead of just telling me what to do. I felt like we worked as a team, and that helped to increase my motivation during my studies. The third part of this project tested the role of the P2X7 receptor in the dentoalveolar morphology of C57B/6 mice. P2X7R KO (knockout) mice were compared to C57B/6 WT to identify differences in a maxillary molar and bone. Tooth dimensions viii were measured and 3D bone morphometry was conducted. No statistically significant differences were found between the two mouse types. P2X7R does not have a major effect on alveolar bone or tooth morphology.The final part examines the role of the P2X7 receptor in a controlled biomechanical model. Orthodontic mechanotransduction was compared in wild-type (WT) and P2X7R knock-out (KO) mice. Using Finite Element Analysis, mouse mechanics were scaled to produce typical human stress levels. Relationships between the biological responses and the calculated stresses were statistically tested and compared.There were direct relationships between certain stress magnitudes and root resorption and bone formation. Hyalinization and root and bone resorption were different in WT and KO. Orthodontic responses are related to the principal stress patterns in the PDL and the P2X7 receptor plays a significant role in their mechanotransduction.

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“…LL-37 is found in the secondary granules of neutrophils (7), is endogenously expressed by a variety of cells including keratinocytes and epithelial cells, and is released in response to multiple inflammatory stimuli (8,9). On release, LL-37 acts as an effector molecule of innate immunity, displaying anti-infective and immunomodulatory activities, including the induction of neutrophil, CD4 + T-cell and monocyte chemotaxis (10), mast cell activation (11), and neutrophil survival (12,13). However, a concentration of 100 μg/mL of LL-37 resulted in the death of 60% untransformed human airway epithelial cells (14).…”

Section: Introductionmentioning

confidence: 99%

“…However, a concentration of 100 μg/mL of LL-37 resulted in the death of 60% untransformed human airway epithelial cells (14). These variations in the cytotoxic nature of LL-37 may potentially be related to peptide-mediated augmentation of innate immunity (13). The ability of LL-37 to promote or inhibit apoptosis depending on the cell type, and the knowledge of other cationic host defense peptides that can kill cancer cells, has led researchers to try and understand the effect(s) of LL-37 on human tumor cells.…”

Section: Introductionmentioning

confidence: 99%

The Human Host Defense Peptide LL-37 Induces Apoptosis in a Calpain- and Apoptosis-Inducing Factor–Dependent Manner Involving Bax Activity

Mader

Mookherjee

Hancock

et al. 2009

Molecular Cancer Research

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LL-37 is a human cationic host defense peptide (antimicrobial peptide) belonging to the cathelicidin family of peptides. In this study, LL-37 was shown to kill Jurkat T leukemia cells via apoptosis. A loss of mitochondrial membrane potential, DNA fragmentation, and phosphatidylserine externalization were detected following LL-37 exposure, whereas apoptosis was independent of caspase family members. The specific apoptotic pathway induced by LL-37 was defined through the utilization of Jurkat cells modified to express antiapoptotic proteins, as well as cells deficient in various proteins associated with apoptosis. Of interest, both Bcl-2-overexpressing cells and cells deficient in Bax and Bak proteins displayed a significant reduction in LL-37-induced apoptosis. In addition, Jurkat cells modified in the Fas receptor-associated pathway showed no reduction in apoptosis when exposed to LL-37. Analysis of the involvement of apoptosis-inducing factor (AIF) in LL-37-mediated apoptosis revealed that AIF transferred from the mitochondria to the nucleus of cells exposed to LL-37, where it may lead to large-scale DNA fragmentation and chromatin condensation. AIF knockdown analysis resulted in LL-37-resistant cells. This suggests that AIF is mandatory in LL-37-mediated killing. Lastly, chelation or inhibition of Ca 2+ or calpains inhibited LL-37-mediated killing. Further analysis revealed that calpains were required for LL-37-mediated Bax translocation to mitochondria. Together, these data show that LL-37-induced apoptosis is mediated via the mitochondria-associated pathway in a caspase-independent and calpain-and AIF-dependent manner that involves Bax activation and translocation to mitochondria. (Mol Cancer Res 2009;7(5):689-702)

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The human cationic host defense peptide LL-37 mediates contrasting effects on apoptotic pathways in different primary cells of the innate immune system

Cited by 147 publications

References 69 publications

Synthetic Cationic Peptide IDR-1002 Provides Protection against Bacterial Infections through Chemokine Induction and Enhanced Leukocyte Recruitment

Synthetic Cationic Peptide IDR-1002 Provides Protection against Bacterial Infections through Chemokine Induction and Enhanced Leukocyte Recruitment

Orthodontic mechanotransduction and the role of the P2X7 receptor

The Human Host Defense Peptide LL-37 Induces Apoptosis in a Calpain- and Apoptosis-Inducing Factor–Dependent Manner Involving Bax Activity

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