KCa and Ca2+ channels: The complex thought

AbstractPotassium channels belong to the largest and the most diverse super-families of ion channels. Among them, Ca2+-activated K+ channels (KCa) comprise many members. Based on their single channel conductance they are divided into three subfamilies: big conductance (BKCa), intermediate conductance (IKCa) and small conductance (SKCa; SK1, SK2 and SK3). Ca2+ channels are divided into two main families, voltage gated/voltage dependent Ca2+ channels and non-voltage gated/voltage independent Ca2+ channels. Based on their electrophysiological and pharmacological properties and on the tissue where there are expressed, voltage gated Ca2+ channels (Cav) are divided into 5 families: T-type, L-type, N-type, P/Q-type and R-type Ca2+. Non-voltage gated Ca2+ channels comprise the TRP (TRPC, TRPV, TRPM, TRPA, TRPP, TRPML and TRPN) and Orai (Orai1 to Orai3) families and their partners STIM (STIM1 to STIM2). A depolarization is needed to activate voltage-gated Ca2+ channels while non-voltage gated Ca2+ channels are activated by Ca2+ depletion of the endoplasmic reticulum stores (SOCs) or by receptors (ROCs). These two Ca2+ channel families also control constitutive Ca2+ entries. For reducing the energy consumption and for the fine regulation of Ca2+, KCa and Ca2+ channels appear associated as complexes in excitable and non-excitable cells. Interestingly, there is now evidence that KCa–Ca2+ channel complexes are also found in cancer cells and contribute to cancer-associated functions such as cell proliferation, cell migration and the capacity to develop metastases. This article is part of a Special Issue entitled: Calcium signaling in health and disease. Guest Editors: Geert Bultynck, Jacques Haiech, Claus W. Heizmann, Joachim Krebs, and Marc Moreau

Activation of TRPV2 and BKCa channels by the LL-37 enantiomers stimulates calcium entry and migration of cancer cells.

International audienceExpression of the antimicrobial peptide hCAP18/LL-37 is associated to malignancy in various cancer forms, stimulating cell migration and metastasis. We report that LL-37 induces migration of three cancer cell lines by activating the TRPV2 calcium-permeable channel and recruiting it to pseudopodia through activation of the PI3K/AKT pathway. Ca2+ entry through TRPV2 cooperated with a K+ efflux through the BKCa channel. In a panel of human breast tumors, the expression of TRPV2 and LL-37 was found to be positively correlated. The D-enantiomer of LL-37 showed identical effects as the L-peptide, suggesting that no binding to a specific receptor was involved. LL-37 attached to caveolae and pseudopodia membranes and decreased membrane fluidity, suggesting that a modification of the physical properties of the lipid membrane bilayer was the underlying mechanism of its effects

Humoral immunity modifications induced by gravity changes

Au cours de ma thèse, j'ai étudié l'impact des stress associés aux vols spatiaux sur l'immunité humorale du pleurodèle et de la souris. Chez le pleurodèle adulte, j'ai d'abord étudié l'utilisation des gènes VH lors de la synthèse des chaînes lourdes d'anticorps suite à une immunisation pendant 5 mois à bord de Mir (expérience Genesis en 1999). J'ai ensuite étudié le processus de maturation de l'affinité des anticorps chez ces mêmes animaux. Ce processus s'effectue par l'apparition d'hypermutations somatiques dans les segments variables des gènes d'anticorps. Ces travaux ont permis de montrer que les segments VH sont utilisés différemment sur Terre et dans Mir et que la fréquence des hypermutations est diminuée suite au vol. Ensuite, j'ai étudié l'impact des stress rencontrés lors d'un autre vol spatial sur la synthèse des premiers anticorps (IgM) chez le pleurodèle en développement (expérience AMPHIBODY en 2006). Le taux d'IgM étant modifié suite à cette expérience, nous avons recréé sur Terre chacun des stress rencontrés en vol (microgravité, hypergravité, choc thermique, radiations, perturbation du rythme circadien et confinement) afin de connaître le(s) stress responsable(s) de cette modification. Ainsi, seule la gravité modifiée affecte l'expression des IgM. Enfin, j'ai étudié l'impact de l'hypergravité (2G et 3G) sur la réponse au stress et le système immunitaire de la souris. Nous avons mis en évidence une réponse physiologique et comportementale au stress à 3G mais pas à 2G. Pourtant, des modifications du système immunitaire sont constatées dès 2G. Cela montre qu'une modification de la gravité, associée ou non à une réponse au stress, affecte le système immunitaireDuring my PhD, I studied the impact of spaceflight-associated stresses on Pleurodeles waltl and Mus musculus humoral immunity. In adult P. waltl immunized during 5 months onboard the Mir space station (Genesis experiment in 1999), I first determined how individual VH genes are used. Then, I studied antibodies affinity maturation in these animals. This maturation implies the introduction of somatic hypermutations (SHM) in DNA encoding the variable segments of antibodies genes. These two pieces of work have shown that variable segments of heavy chain gene are differently used and that SHM frequency is reduced when immunization occurs in space. Then, I studied antibodies production during animal development onboard the international space station (ISS) (AMPHIBODY experiment in 2006). The antibodies production being increased in larvae that developed in the ISS, we recreated in the laboratory each stress encountered during the spaceflight (hypergravity, microgravity, heat shock associated to the re-entry in the atmosphere, radiations, perturbation of circadian rhythm and confinement) to determine their impact on IgM heavy chain transcription. This allowed to observe that only gravity changes affect this transcription. Finally, I studied the impact of hypergravity (2G and 3G) on the murine immune system. I observed physiological and behavioural stress responses in mice exposed to 3G but not in 2G mice. However, immune system alterations were observed in both the 2G and 3G groups, suggesting that gravity modifications, associated or not with stress responses, are responsible for immune system modification

Modifications de l'immunité humorale induites par des changements de la gravité

During my PhD, I studied the impact of spaceflight-associated stresses on Pleurodeles waltl and Mus musculus humoral immunity. In adult P. waltl immunized during 5 months onboard the Mir space station (Genesis experiment in 1999), I first determined how individual VH genes are used. Then, I studied antibodies affinity maturation in these animals. This maturation implies the introduction of somatic hypermutations (SHM) in DNA encoding the variable segments of antibodies genes. These two pieces of work have shown that variable segments of heavy chain gene are differently used and that SHM frequency is reduced when immunization occurs in space. Then, I studied antibodies production during animal development onboard the international space station (ISS) (AMPHIBODY experiment in 2006). The antibodies production being increased in larvae that developed in the ISS, we recreated in the laboratory each stress encountered during the spaceflight (hypergravity, microgravity, heat shock associated to the re-entry in the atmosphere, radiations, perturbation of circadian rhythm and confinement) to determine their impact on IgM heavy chain transcription. This allowed to observe that only gravity changes affect this transcription. Finally, I studied the impact of hypergravity (2G and 3G) on the murine immune system. I observed physiological and behavioural stress responses in mice exposed to 3G but not in 2G mice. However, immune system alterations were observed in both the 2G and 3G groups, suggesting that gravity modifications, associated or not with stress responses, are responsible for immune system modificationsAu cours de ma thèse, j'ai étudié l'impact des stress associés aux vols spatiaux sur l'immunité humorale du pleurodèle et de la souris. Chez le pleurodèle adulte, j'ai d'abord étudié l'utilisation des gènes VH lors de la synthèse des chaînes lourdes d'anticorps suite à une immunisation pendant 5 mois à bord de Mir (expérience Genesis en 1999). J'ai ensuite étudié le processus de maturation de l'affinité des anticorps chez ces mêmes animaux. Ce processus s'effectue par l'apparition d'hypermutations somatiques dans les segments variables des gènes d'anticorps. Ces travaux ont permis de montrer que les segments VH sont utilisés différemment sur Terre et dans Mir et que la fréquence des hypermutations est diminuée suite au vol. Ensuite, j'ai étudié l'impact des stress rencontrés lors d'un autre vol spatial sur la synthèse des premiers anticorps (IgM) chez le pleurodèle en développement (expérience AMPHIBODY en 2006). Le taux d'IgM étant modifié suite à cette expérience, nous avons recréé sur Terre chacun des stress rencontrés en vol (microgravité, hypergravité, choc thermique, radiations, perturbation du rythme circadien et confinement) afin de connaître le(s) stress responsable(s) de cette modification. Ainsi, seule la gravité modifiée affecte l'expression des IgM. Enfin, j'ai étudié l'impact de l'hypergravité (2G et 3G) sur la réponse au stress et le système immunitaire de la souris. Nous avons mis en évidence une réponse physiologique et comportementale au stress à 3G mais pas à 2G. Pourtant, des modifications du système immunitaire sont constatées dès 2G. Cela montre qu'une modification de la gravité, associée ou non à une réponse au stress, affecte le système immunitair

Zellen des Immunsystems: vom Polarkreis ins All

Das Immunsystem gehört auf einem Raumflug zu den am stärksten beeinträchtigten Systemen des menschlichen Körpers. Die Ursache dieser Störung liegt wahrscheinlich auf Ebene der Zellen. Experimente an Bord einer TEXUS-Forschungsrakete sollen nun Aufschluss hierüber geben. Abstract: Immune system malfunction is one of the major limiting factors for human health and performance during space flight. Experiments on board of the TEXUS-49 rocket were carried out to shed light on the underlying molecular alterations

Modulation of Iberian Ribbed Newt Complement Component C3 by Stressors Similar to those Encountered during a Stay Onboard the International Space Station

The complement system plays an important role in inflammation, innate and acquired immunity, as well as homeostasis. Despite these functions, the effects of spaceflight conditions on the complement system have not yet been intensively studied. Consequently, we investigated the effects of five types of chronic stressors, similar to those encountered during a stay onboard the International Space Station, on C3 expression in larvae of the urodele amphibian Pleurodeles waltl. We focused on C3 because it is a critical component of this system. These studies were completed by the analysis of adult mice exposed to two models of inflight stressors. Our data show that simulating space radiation, or combining a modification of the circadian rhythm with simulated microgravity, affects the amount of C3 proteins. These results suggest that C3 expression could be modified under real spaceflight conditions, potentially increasing the risk of inflammation and associated tissue damage

Calcium Signaling Is Dispensable for Receptor Regulation of Endothelial Barrier Function

International audienc

L’échangeur ionique NCLX : Un rôle ambivalent dans la chronologie du cancer colorectal

International audienceNo abstract availabl