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BBA - Biomembranes (v.1719, #1-2)
Connexins, innexins and pannexins: Bridging the communication gap
by Jean-Claude Hervé; Pauline Phelan; Roberto Bruzzone; Thomas W. White (pp. 3-5).
Regulation of connexin expression by Masahito Oyamada; Yumiko Oyamada; Tetsuro Takamatsu (pp. 6-23).
Gap junctions contain cell–cell communicating channels that consist of multimeric proteins called connexins and mediate the exchange of low-molecular-weight metabolites and ions between contacting cells. Gap junctional communication has long been hypothesized to play a crucial role in the maintenance of homeostasis, morphogenesis, cell differentiation, and growth control in multicellular organisms. The recent discovery that human genetic disorders are associated with mutations in connexin genes and experimental data on connexin knockout mice have provided direct evidence that gap junctional communication is essential for tissue functions and organ development. Thus far, 21 human genes and 20 mouse genes for connexins have been identified. Each connexin shows tissue- or cell-type-specific expression, and most organs and many cell types express more than one connexin. Cell coupling via gap junctions is dependent on the specific pattern of connexin gene expression. This pattern of gene expression is altered during development and in several pathological conditions resulting in changes of cell coupling. Connexin expression can be regulated at many of the steps in the pathway from DNA to RNA to protein. However, transcriptional control is one of the most important points. In this review, we summarize recent knowledge on transcriptional regulation of connexin genes by describing the structure of connexin genes and transcriptional factors that regulate connexin expression.
Keywords: Connexin; Gap junction; Gene regulation; Alternative splicing; Transcription factor
Temporal regulation of connexin phosphorylation in embryonic and adult tissues by Timothy J. King; Paul D. Lampe (pp. 24-35).
Gap junctions, composed of proteins from the connexin family, allow for intercellular communication between cells in tissues and are important in development, tissue/cellular homeostasis, and carcinogenesis. Genome databases indicate that there are at least 20 connexins in the mouse and human. Connexin phosphorylation has been implicated in connexin assembly into gap junctions, gap junction turnover, and cell signaling events that occur in response to tumor promoters and oncogenes. Connexin43 (Cx43), the most widely expressed and abundant gap junction protein, can be phosphorylated at several different serine and tyrosine residues. Here, we focus on the dynamic regulation of Cx43 phosphorylation in tissue and how these regulatory events are affected during development, wound healing, and carcinogenesis. The activation of several kinases, including protein kinase A, protein kinase C, p34cdc2/cyclin B kinase, casein kinase 1, mitogen-activated protein kinase, and pp60src kinase, can lead to the phosphorylation of different residues in the C-terminal region of Cx43. The use of antibodies specific for phosphorylation at defined residues has allowed the examination of specific phosphorylation events both in tissue culture and in vivo. These new antibody tools and those under development will allow us to correlate specific phosphorylation events with changes in connexin function.
Keywords: Abbreviations; Cx; connexin; MAPK; mitogen-activated protein kinase; PKC; protein kinase C; TPA; 12-; O; -tetradeconylphorbol-13-acetate; NP; non-phosphorylated; SDS-PAGE; sodium dodecylsulfate-polyacrylamide gel electrophoresisConnexin; Gap junction; Phosphorylation; Phosphospecific antibody; Cell signalling
Pharmacology of Gap junctions. New pharmacological targets for treatment of arrhythmia, seizure and cancer? by Aida Salameh; Stefan Dhein (pp. 36-58).
Intercellular communication in many organs is maintained via intercellular gap junction channels composed of connexins, a large protein family with a number of isoforms. This gap junction intercellular communication (GJIC) allows the propagation of action potentials (e.g., in brain, heart), and the transfer of small molecules which may regulate cell growth, differentiation and function. The latter has been shown to be involved in cancer growth: reduced GJIC often is associated with increased tumor growth or with de-differentiation processes. Disturbances of GJIC in the heart can cause arrhythmia, while in brain electrical activity during seizures seems to be propagated via gap junction channels. Many diseases or pathophysiological conditions seem to be associated with alterations of gap junction protein expression. Thus, depending on the target disease opening or closure of gap junctions may be of interest, or alteration of connexin expression. GJIC can be affected acutely by changing gap junction conductance or – more chronic – by altering connexin expression and membrane localisation. This review gives an overview on drugs affecting GJIC.
Keywords: Gap junction; Connexin; Intercellular communication; Pharmacology; Toxicology; Cardiac; Cancer; Seizure
Involvement of gap junctions in the development of the neocortex by Bernd Sutor; Timothy Hagerty (pp. 59-68).
Gap junctions play an important role during the development of the mammalian brain. In the neocortex, gap junctions are already expressed at very early stages of development and they seem to be involved in many processes like neurogenesis, migration and synapse formation. Gap junctions are found in all cell types including progenitor cells, glial cells and neurons. These direct cell-to-cell connections form clusters consisting of a distinct number of cells of a certain type. These clusters can be considered as communication compartments in which the information transfer is mediated electrically by ionic currents and/or chemically by, e.g., small second messenger molecules. Within the neocortex, four such communication compartments can be identified: (1) gap junction-coupled neuroblasts of the ventricular zone and gap junctions in migrating cells and radial glia, (2) gap junction-coupled glial cells (astrocytes and oligodendrocytes), (3) gap junction-coupled pyramidal cells (only during the first two postnatal weeks) and (4) gap junction-coupled inhibitory interneurons. These compartments can consist of sub-compartments and they may overlap to some degree. The compartments 1 and 3 disappear with ongoing develop, whereas compartments 2 and 4 persist in the mature neocortex. Gap junction-mediated coupling of glial cells seems to be important for stabilization of the extracellular ion homeostasis, uptake of neurotransmitters, migration of neurons and myelination of axons. Electrical synapses between inhibitory interneurons facilitate the synchronization of pyramidal cells. In this way, they contribute to the generation of oscillatory network activity correlated with higher cortical functions. The role of gap junctions present in neuroblasts of the ventricular zone as well as the role of gap junctions found in pyramidal cells during the early postnatal stages is less clear. It is assumed that they might help to form precursors of the functional columns observed in the mature neocortex. Although recent developments of new techniques led to the solution of many problems concerning gap junction-coupling between neurons and glial cells in the neocortex, there are many open questions which need to be answered before we can achieve a comprehensive understanding of the role of gap junctions in the development of the neocortex.
Keywords: Gap junction; Neocortex; Development; Interneuron; Pyramidal cell; Glia
Gap junctions in skeletal development and function by Joseph P. Stains; Roberto Civitelli (pp. 69-81).
Gap junctions play a critical role in the coordinated function and activity of nearly all of the skeletal cells. This is not surprising, given the elaborate orchestration of skeletal patterning, bone modeling and subsequent remodeling, as well as the mechanical stresses, strains and adaptive responses that the skeleton must accommodate. Much remains to be learned regarding the role of gap junctions and hemichannels in these processes. A common theme is that without connexins none of the cells of bone function properly. Thus, connexins play an important role in skeletal form and function.
Keywords: Connexin; Bone; Cartilage; Osteoblast; Chondrocyte
Involvement of gap junctional communication in secretion by Laetitia Michon; Rachel Nlend Nlend; Sabine Bavamian; Lorraine Bischoff; Nathalie Boucard; Dorothée Caille; José Cancela; Anne Charollais; Eric Charpantier; Philippe Klee; Manon Peyrou; Céline Populaire; Laurence Zulianello; Paolo Meda (pp. 82-101).
Glands were the first type of tissues in which the permissive role of gap junctions in the cell-to-cell transfer of membrane-impermeant molecules was shown. During the 40 years that have followed this seminal finding, gap junctions have been documented in all types of multicellular secretory systems, whether of the exocrine, endocrine or pheromonal nature. Also, compelling evidence now indicates that gap junction-mediated coupling, and/or the connexin proteins per se, play significant regulatory roles in various aspects of gland functions, ranging from the biosynthesis, storage and release of a variety of secretory products, to the control of the growth and differentiation of secretory cells, and to the regulation of gland morphogenesis. This review summarizes this evidence in the light of recent reports.
Keywords: Exocrine gland; Endocrine gland; Enzyme; Hormone; Ca; 2+; Synchronization
Gap junctional communication in the male reproductive system by Georges Pointis; Céline Fiorini; Norah Defamie; Dominique Segretain (pp. 102-116).
Male fertility is a highly controlled process that allows proliferation, meiosis and differentiation of male germ cells in the testis, final maturation in the epididymis and also requires functional male accessory glands: seminal vesicles, prostate and corpus cavernosum. In addition to classical endocrine and paracrine controls, mainly by gonadotropins LH and FSH and steroids, there is now strong evidence that all these processes are dependent upon the presence of homocellular or heterocellular junctions, including gap junctions and their specific connexins (Cxs), between the different cell types that structure the male reproductive tract. The present review is focused on the identification of Cxs, their distribution in the testis and in different structures of the male genital tract (epididymis, seminal vesicle, prostate, corpus cavernosum), their crucial role in the control of spermatogenesis and their implication in the function of the male accessory glands, including functional smooth muscle tone. Their potential dysfunctions in some testis (spermatogenic arrest, seminoma) and prostate (benign hyperplasia, adenocarcinoma) diseases and in the physiopathology of the human erectile function are also discussed.
Keywords: Gap junction; Connexin; Male reproductive tract; Fertility; Pathogenesis
Involvement of gap junctions in placental functions and development by A. Malassiné; L. Cronier (pp. 117-124).
Connexin (Cx) expression and gap junctional intercellular communication (GJIC) are involved in development and differentiation processes. Mediating exchanges between mother and fetus, the placenta is formed when fetal membranes are apposed or even fusing or destroying the uterine mucosa. Therefore, an extraordinary variability of placental structures is observed throughout the mammalian species. This variability affect mainly, the maternofetal blood flow interrelationships, the kind and number of tissue layers separating maternal and fetal bloods, the trophoblast invasiveness and the formation of a syncytium (syncytiotrophoblast). Here, the expression, the localisation and the possible role of Cx and GJIC in placental functions and development are discussed.In rodents, gene knock out in mice have vastly improved our understanding of the role of Cx genes in mouse placental development: Cx26 in transplacental uptake of glucose, Cx31 in the proliferative process of trophoblastic cells and Cx45 in placental vascularisation. In human, it appears that Cx43 allows a GJIC required for the fusion process of cytotrophoblastic cells leading to the formation of the syncytiotrophoblast, the site of the numerous placental functions. On other hands, Cx40 plays a critical role in the switch from a proliferative to an invasive phenotype of the trophoblastic cells invading the endometrium. Owing to the striking diversity of Cx expression in placental structures, we must be careful when extrapolating findings from one species to another.
Keywords: Gap junction; Placenta; Trophoblast; Connexin; Cell–cell communication; Differentiation processe
Defective gap junctional intercellular communication in the carcinogenic process by Marc Mesnil; Sophie Crespin; José-Luis Avanzo; Maria-Lucia Zaidan-Dagli (pp. 125-145).
Gap junctions are membrane structures made of intercellular channels which permit the diffusion from cytoplasm to cytoplasm of small hydrophilic molecules. Nearly 40 years ago, the loss of functional gap junctions has been described in cancer cells and led to the hypothesis that such type of intercellular communication is involved in the carcinogenesis process. From this time, a lot of data has been accumulated confirming that gap junctions are frequently decreased or absent in cancer cells whatever their tissue and species origins. Here, we review such data by insisting on the possible links existing between altered gap-junctional intercellular communication capacity (or the altered expression of their constitutive proteins, the connexins) and the stages of cancer progression in various cancer models. Then, we analyse particular aspects of the disturbance of connexin-mediated communication in cancer such as the cytoplasmic localization of connexins, the lack of heterologous communication between cancer cells and normal cells, the role of connexin gene mutations in cancer. In a separate part of the review, we also analyse the disturbance of gap-junctional intercellular communication during the late stages of cancer (invasion and metastasis processes).
Keywords: Cancer; Carcinogenesis; Connexin; Gap junction; Gap-junctional intercellular communication
Connexins as targets for cancer chemoprevention and chemotherapy by Timothy J. King; John S. Bertram (pp. 146-160).
Cells within a tissue continuously interact to coordinate normal tissue functions and maintain homeostasis. Gap junctional communication (GJC), mediated by the connexin protein family, allows this type of intercellular crosstalk resulting in synchronized and cooperative tissue behavior such as cardiac contraction. In cancer, loss of these types of cell:cell interactions has been shown to facilitate tumorigenesis and enable the autonomous cell behavior associated with transformed cells. Indeed, many human tumor lines demonstrate deficient or aberrant GJC and/or loss of connexin expression. Restoration of exogenous connexin expression/GJC function is correlated with increased cell growth control both in vitro and in vivo. In support of this growth regulatory hypothesis, decreased connexin expression has been observed in situ in early human neoplasia of various organs. Additionally, genetically engineered mice lacking particular connexins (Connexins 32 or 43) exhibit increased susceptibility to radiation and chemically-induced liver and/or lung tumorigenesis. These studies strongly suggest that connexins and GJC serve a tumor suppressor role. Consistent with this proposed role, in a model cell culture system, retinoids and carotenoids up-regulate Connexin43 (Cx43) expression in direct proportion to their ability to suppress carcinogen-induced neoplastic transformation. Here, we discuss the important role of connexins and GJC in tumorigenesis and suggest the possibility of connexins as potential anti-oncogenic targets for chemoprevention and/or chemotherapy.
Keywords: Connexin; Gap junction; Chemoprevention; Chemotherapy; Cancer