Your search keyword '"Solan JL"' showing total 35 results

1. Changes in connexin43 expression and localization during pancreatic cancer progression.

Author

Solan JL, Hingorani SR, Lampe PD, Solan, Joell L, Hingorani, Sunil R, and Lampe, Paul D

Abstract

Gap junctions and gap junction communication have long been recognized to play roles in tissue organization and remodeling through both cell autonomous and intercellular means. We hypothesized that these processes become dysregulated during pancreas cancer progression. Molecular and histological characterization of the gap junction protein, connexin43, during progression of pancreatic ductal adenocarcinoma could yield insight into how these events may contribute to or be modulated during carcinogenesis. In a mouse model of pancreatic ductal adenocarcinoma generated through targeted endogenous expression of Kras(G12D) in the murine pancreas, we examined the evolving expression and localization of connexin43. Overall, connexin43 expression increased over time, and its localization became more widespread. At early stages, connexin43 is found almost exclusively in association with the basolateral membrane of duct cells found in invasive lesions. Connexin43 became increasingly associated with the surrounding stroma over time. Connexin43 phosphorylation was also altered during tumorigenesis, as assessed by migrational changes of the protein in immunoblots. These data suggest a potential role for gap junctions and connexin43 in mediating interactions between and amongst the stromal and epithelial cells in pancreatic ductal adenocarcinoma. [ABSTRACT FROM AUTHOR]

Published

2012

2. Transport of Connexins and Gap Junction Turnover in Living Cells Visualized Using Green Fluorescent Protein Tagged Connexins.

Author

Bailey, GW, Jerome, WG, McKernan, S, Mansfield, JF, Price, RL, Laird, DW, Jordan, K, Fistouris, P, Solan, JL, Lampe, PD, and Shao, C

Published

1999

3. Transport of Connexins and Gap Junction Turnover in Living Cells Visualized Using Green Fluorescent Protein Tagged Connexins.

Author

Laird, DW, Jordan, K, Fistouris, P, Solan, JL, Lampe, PD, and Shao, C

Abstract

Connexins oligomerize into hemichannels, traffic to the cell surface and dock with hemichannels from an adjacent cell to form intercellular gap junction channels. Pulsechase studies have revealed that connexins are subject to a short half-life ranging from 1- 5 hrs. To examine the mechanisms involved in connexin trafficking, gap junction assembly and internalization in living cells we fused green fluorescent protein (GFP) to the amino or carboxyl terminus of full length connexins (Cx). When cDNA encoding Cx43-GFP was transfected into communication-competent NRK cells, Cx43-negative MDCK cells, or communication-deficient Neuro2A or HeLa cells, the fusion protein of predicted length was expressed, transported, and assembled into functional gap junctions (Figure 1). Most notably, the fusion of GFP to the amino terminal of Cx43 (GFP-Cx43) or Cx32 (GFP-Cx32) did not inhibit the co-translational insertion of these polytopic type IV connexins into the membrane and as a result gap junction plaques assembled at cellcell interfaces.

Published

1999

4. Casein Kinase 1 Phosphomimetic Mutations Negatively Impact Connexin-43 Gap Junctions in Human Pluripotent Stem Cell-Derived Cardiomyocytes.

Author

Al-Attar R, Jargstorf J, Romagnuolo R, Jouni M, Alibhai FJ, Lampe PD, Solan JL, and Laflamme MA

Subjects

Adult, Animals, Humans, Mice, Connexins, Gap Junctions, Mice, Transgenic, Mutation, Casein Kinase I genetics, Connexin 43 genetics, Myocytes, Cardiac

Abstract

The transplantation of human pluripotent stem cell-derived cardiomyocytes (hPSC-CMs) has shown promise in preclinical models of myocardial infarction, but graft myocardium exhibits incomplete host-graft electromechanical integration and a propensity for pro-arrhythmic behavior. Perhaps contributing to this situation, hPSC-CM grafts show low expression of connexin 43 (Cx43), the major gap junction (GJ) protein, in ventricular myocardia. We hypothesized that Cx43 expression and function could be rescued by engineering Cx43 in hPSC-CMs with a series of phosphatase-resistant mutations at three casein kinase 1 phosphorylation sites (Cx43-S3E) that have been previously reported to stabilize Cx43 GJs and reduce arrhythmias in transgenic mice. However, contrary to our predictions, transgenic Cx43-S3E hPSC-CMs exhibited reduced Cx43 expression relative to wild-type cells, both at baseline and following ischemic challenge. Cx43-S3E hPSC-CMs showed correspondingly slower conduction velocities, increased automaticity, and differential expression of other connexin isoforms and various genes involved in cardiac excitation-contraction coupling. Cx43-S3E hPSC-CMs also had phosphorylation marks associated with Cx43 GJ internalization, a finding that may account for their impaired GJ localization. Taken collectively, our data indicate that the Cx43-S3E mutation behaves differently in hPSC-CMs than in adult mouse ventricular myocytes and that multiple biological factors likely need to be addressed synchronously to ensure proper Cx43 expression, localization, and function.

Published

2024

5. Posttranslational modifications induce autoantibodies with risk prediction capability in patients with small cell lung cancer.

Author

Lastwika KJ, Kunihiro A, Solan JL, Zhang Y, Taverne LR, Shelley D, Rho JH, Randolph TW, Li CI, Grogan EL, Massion PP, Fitzpatrick AL, MacPherson D, Houghton AM, and Lampe PD

Subjects

Humans, Autoantibodies, Protein Processing, Post-Translational, Small Cell Lung Carcinoma, Lung Neoplasms pathology

Abstract

Small cell lung cancer (SCLC) elicits the generation of autoantibodies that result in unique paraneoplastic neurological syndromes. The mechanistic basis for the formation of such autoantibodies is largely unknown but is key to understanding their etiology. We developed a high-dimensional technique that enables detection of autoantibodies in complex with native antigens directly from patient plasma. Here, we used our platform to screen 1009 human plasma samples for 3600 autoantibody-antigen complexes, finding that plasma from patients with SCLC harbors, on average, fourfold higher disease-specific autoantibody signals compared with plasma from patients with other cancers. Across three independent SCLC cohorts, we identified a set of common but previously unknown autoantibodies that are produced in response to both intracellular and extracellular tumor antigens. We further characterized several disease-specific posttranslational modifications within extracellular proteins targeted by these autoantibodies, including citrullination, isoaspartylation, and cancer-specific glycosylation. Because most patients with SCLC have metastatic disease at diagnosis, we queried whether these autoantibodies could be used for SCLC early detection. We created a risk prediction model using five autoantibodies with an average area under the curve of 0.84 for the three cohorts that improved to 0.96 by incorporating cigarette smoke consumption in pack years. Together, our findings provide an innovative approach to identify circulating autoantibodies in SCLC with mechanistic insight into disease-specific immunogenicity and clinical utility.

Published

2023

6. CD133 as a Biomarker for an Autoantibody-to-ImmunoPET Paradigm for the Early Detection of Small Cell Lung Cancer.

Author

Kunihiro AG, Sarrett SM, Lastwika KJ, Solan JL, Pisarenko T, Keinänen O, Rodriguez C, Taverne LR, Fitzpatrick AL, Li CI, Houghton AM, Zeglis BM, and Lampe PD

Subjects

Animals, Humans, Mice, Positron-Emission Tomography methods, Mice, Nude, Early Detection of Cancer, Disease Models, Animal, Biomarkers, Autoantibodies, RNA, Messenger, Cell Line, Tumor, Small Cell Lung Carcinoma metabolism, Lung Neoplasms metabolism, Neuroendocrine Tumors

Abstract

Small cell lung cancer (SCLC) is a deadly neuroendocrine tumor for which there are no screening methods sensitive enough to facilitate early, effective intervention. We propose targeting the neuroendocrine tumor neoantigen CD133 via antibody-based early detection and PET (immunoPET) to facilitate earlier and more accurate detection of SCLC. Methods: RNA sequencing datasets, immunohistochemistry, flow cytometry, and Western blots were used to quantify CD133 expression in healthy and SCLC patients. CD133 was imaged in vivo using near-infrared fluorescence (NIRF) immunoimaging, and 89 Zr immunoPET. Anti(α)-CD133 autoantibody levels were measured in SCLC patient plasma using antibody microarrays. Results: Across 6 publicly available datasets, CD133 messenger RNA was found to be higher in SCLC tumors than in other tissues, including healthy or normal adjacent lung and non-SCLC samples. Critically, the upregulation of CD133 messenger RNA in SCLC was associated with a significant increase (hazard ratio, 2.62) in death. CD133 protein was expressed in primary human SCLC, in SCLC patient-derived xenografts, and in both SCLC cell lines tested (H82 and H69). Using an H82 xenograft mouse model, we first imaged CD133 expression with NIRF. Both in vivo and ex vivo NIRF clearly showed that a fluorophore-tagged αCD133 homed to lung tumors. Next, we validated the noninvasive visualization of subcutaneous and orthotopic H82 xenografts via immunoPET. An αCD133 antibody labeled with the positron-emitting radiometal 89 Zr demonstrated significant accumulation in tumor tissue while producing minimal uptake in healthy organs. Finally, plasma αCD133 autoantibodies were found in subjects from cohort studies up to 1 year before SCLC diagnosis. Conclusion: In light of these findings, we conclude that the presence of αCD133 autoantibodies in a blood sample followed by CD133-targeted 89 Zr-immunoPET could be an effective early detection screening strategy for SCLC., (© 2022 by the Society of Nuclear Medicine and Molecular Imaging.)

Published

2022

7. Cx43 phosphorylation sites regulate pancreatic cancer metastasis.

Author

Solan JL, Hingorani SR, and Lampe PD

Subjects

Adenocarcinoma pathology, Animals, Carcinogenesis genetics, Carcinoma, Pancreatic Ductal pathology, Cell Proliferation genetics, Gap Junctions genetics, Gap Junctions pathology, Humans, Interferon-Stimulated Gene Factor 3, gamma Subunit genetics, Mice, Neoplasm Metastasis, Phosphorylation genetics, Adenocarcinoma genetics, Carcinoma, Pancreatic Ductal genetics, Casein Kinase I genetics, Connexin 43 genetics, Proto-Oncogene Proteins p21(ras) genetics

Abstract

Pancreatic ductal adenocarcinoma (PDA) is aggressive, highly metastatic and characterized by a robust desmoplasia. Connexin proteins that form gap junctions have been implicated in tumor suppression for over 30 years. Cx43, the most widely expressed connexin, regulates cell behaviors, including migration and proliferation. Thus, we hypothesized that Cx43 could regulate PDA progression. Phosphorylation of Cx43 by Casein Kinase 1 (CK1) regulates gap junction assembly. We interbred the well-established Kras LSL-G12D/+;p48Cre/+ (KC) mouse model of PDA with homozygous "knock-in" mutant Cx43 mice bearing amino acid substitution at CK1 sites (Cx43 CK1A ) and found profound and surprising effects on cancer progression. Crossing the Cx43 CK1A mouse onto the KC background (termed KC;Cx CK1A ) led to significant extension of lifespan, from a median of 370 to 486 days (p = 0.03) and a decreased incidence of metastasis (p = 0.045). However, when we examined early stages of disease, we found more rapid onset of tissue remodeling in the KC;Cx CK1A mouse followed by divergence to a cystic phenotype. During tumorigenesis, gap junctions are increasingly present in stromal cells of the KC mice but are absent from the KC;Cx43 CK1A mice. Tail vein metastasis assays with cells derived from KC or KC;Cx CK1A tumors showed that KC;Cx CK1A cells could efficiently colonize the lung and downregulate Cx43 expression, arguing that inhibition of metastasis was not occurring at the distal site. Instead, stromal gap junctions, their associated signaling events or other unknown Cx43-dependent events facilitate metastatic capacity in the primary tumor.

Published

2021

8. Correction to: Optical mapping of human embryonic stem cell-derived cardiomyocyte graft electrical activity in injured hearts.

Author

Filice D, Dhahri W, Solan JL, Lampe PD, Steele E, Milani N, Van Biber B, Zhu WZ, Valdman TS, Romagnuolo R, Otero-Cruz JD, Hauch KD, Kay MW, Sarvazyan N, and Laflamme MA

Published

2021

9. Src Regulation of Cx43 Phosphorylation and Gap Junction Turnover.

Author

Solan JL and Lampe PD

Subjects

Animals, Cell Line, Phosphorylation, Rats, Connexin 43 metabolism, Gap Junctions metabolism, src-Family Kinases metabolism

Abstract

The gap junction protein Connexin43 (Cx43) is highly regulated by phosphorylation at over a dozen sites by probably at least as many kinases. This Cx43 "kinome" plays an important role in gap junction assembly and turnover. We sought to gain a better understanding of the interrelationship of these phosphorylation events particularly related to src activation and Cx43 turnover. Using state-of-the-art live imaging methods, specific inhibitors and many phosphorylation-status specific antibodies, we found phospho-specific domains in gap junction plaques and show evidence that multiple pathways of disassembly exist and can be regulated at the cellular and subcellular level. We found Src activation promotes formation of connexisomes (internalized gap junctions) in a process involving ERK-mediated phosphorylation of S279/282. Proteasome inhibition dramatically and rapidly restored gap junctions in the presence of Src and led to dramatic changes in the Cx43 phospho-profile including to increased Y247, Y265, S279/282, S365, and S373 phosphorylation. Lysosomal inhibition, on the other hand, nearly eliminated phosphorylation on Y247 and Y265 and reduced S368 and S373 while increasing S279/282 phosphorylation levels. We present a model of gap junction disassembly where multiple modes of disassembly are regulated by phosphorylation and can have differential effects on cellular signaling.

Published

2020

10. Optical mapping of human embryonic stem cell-derived cardiomyocyte graft electrical activity in injured hearts.

Author

Filice D, Dhahri W, Solan JL, Lampe PD, Steele E, Milani N, Van Biber B, Zhu WZ, Valdman TS, Romagnuolo R, Otero-Cruz JD, Hauch KD, Kay MW, Sarvazyan N, and Laflamme MA

Subjects

Animals, Cell Differentiation, Embryonic Stem Cells, Guinea Pigs, Myocardium, Human Embryonic Stem Cells, Myocytes, Cardiac

Abstract

Background: Human embryonic stem cell-derived cardiomyocytes (hESC-CMs) show tremendous promise for cardiac regeneration, but the successful development of hESC-CM-based therapies requires improved tools to investigate their electrical behavior in recipient hearts. While optical voltage mapping is a powerful technique for studying myocardial electrical activity ex vivo, we have previously shown that intra-cardiac hESC-CM grafts are not labeled by conventional voltage-sensitive fluorescent dyes. We hypothesized that the water-soluble voltage-sensitive dye di-2-ANEPEQ would label engrafted hESC-CMs and thereby facilitate characterization of graft electrical function and integration., Methods: We developed and validated a novel optical voltage mapping strategy based on the simultaneous imaging of the calcium-sensitive fluorescent protein GCaMP3, a graft-autonomous reporter of graft activation, and optical action potentials (oAPs) derived from di-2-ANEPEQ, which labels both graft and host myocardium. Cardiomyocytes from three different GCaMP3+ hESC lines (H7, RUES2, or ESI-17) were transplanted into guinea pig models of subacute and chronic infarction, followed by optical mapping at 2 weeks post-transplantation., Results: Use of a water-soluble voltage-sensitive dye revealed pro-arrhythmic properties of GCaMP3+ hESC-CM grafts from all three lines including slow conduction velocity, incomplete host-graft coupling, and spatially heterogeneous patterns of activation that varied beat-to-beat. GCaMP3+ hESC-CMs from the RUES2 and ESI-17 lines both showed prolonged oAP durations both in vitro and in vivo. Although hESC-CMs partially remuscularize the injured hearts, histological evaluation revealed immature graft structure and impaired gap junction expression at this early timepoint., Conclusion: Simultaneous imaging of GCaMP3 and di-2-ANEPEQ allowed us to acquire the first unambiguously graft-derived oAPs from hESC-CM-engrafted hearts and yielded critical insights into their arrhythmogenic potential and line-to-line variation.

Published

2020

11. The lipidated connexin mimetic peptide SRPTEKT- Hdc is a potent inhibitor of Cx43 channels with specificity for the pS368 phospho-isoform.

Author

Cotter ML, Boitano S, Lampe PD, Solan JL, Vagner J, Ek-Vitorin JF, and Burt JM

Subjects

Adenosine Triphosphate metabolism, Animals, Calcium metabolism, Cells, Cultured, Connexins metabolism, Dogs, Madin Darby Canine Kidney Cells, Oligopeptides, Protein Isoforms metabolism, Connexin 43 metabolism, Gap Junctions metabolism, Ion Channels metabolism, Peptides metabolism

Abstract

Connexin (Cx) mimetic peptides derived from extracellular loop II sequences (e.g., Gap27: SRPTEKTIFII; Peptide5: VDCFLSRPTEKT) have been used as reversible, Cx-specific blockers of hemichannel (HCh) and gap junction channel (GJCh) function. These blockers typically require high concentrations (~5 µM, <1 h for HCh; ~100 µM, >1 h for GJCh) to achieve inhibition. We have shown that addition of a hexadecyl ( Hdc ) lipid tail to the conserved SRPTEKT peptide sequence (SRPTEKT- Hdc ) results in a novel, highly efficacious, and potent inhibitor of mechanically induced Ca 2+ -wave propagation (IC 50 64.8 pM) and HCh-mediated dye uptake (IC 50 45.0 pM) in Madin-Darby canine kidney cells expressing rat Cx43 (MDCK43). The lack of similar effect on dye coupling (NBD-MTMA) suggested channel conformation-specific inhibition. Here we report that SRPTEKT- Hdc inhibition of Ca 2+ -wave propagation, dye coupling, and dye uptake depended on the functional configuration of Cx43 as determined by phosphorylation at serine 368 (S368). Ca 2+ -wave propagation was enhanced in MDCK cells expressing single-site mutants of Cx43 that mimicked (MDCK43-S368D) or favored (MDCK43-S365A) phosphorylation at S368. Furthermore, SRPTEKT- Hdc potently inhibited GJCh-mediated Ca 2+ -wave propagation (IC 50 230.4 pM), dye coupling, and HCh-mediated dye uptake in MDCK43-S368D and -S365A cells. In contrast, Ca 2+ -wave propagation, dye coupling, and dye uptake were largely unaffected (IC 50 12.3 μM) by SRPTEKT- Hdc in MDCK43-S368A and -S365D cells, mutations that mimic or favor dephosphorylation at S368. Together, these data indicate that SRPTEKT- Hdc is a potent inhibitor of physiological Ca 2+ -wave signaling mediated specifically by the pS368 phosphorylated form of Cx43.

Published

2019

12. Phosphorylation of connexin 43 at MAPK, PKC or CK1 sites each distinctly alter the kinetics of epidermal wound repair.

Author

Lastwika KJ, Dunn CA, Solan JL, and Lampe PD

Subjects

Animals, Casein Kinase I genetics, Cell Line, Connexin 43 genetics, Dogs, Epidermal Cells, Immunohistochemistry, Kinetics, Mice, Mitogen-Activated Protein Kinases genetics, Phosphorylation genetics, Protein Kinase C genetics, Casein Kinase I metabolism, Connexin 43 metabolism, Mitogen-Activated Protein Kinases metabolism, Phosphorylation physiology, Protein Kinase C metabolism

Abstract

The gap junction protein connexin 43 (Cx43) is a key player in wound healing, and inhibitors of Cx43, which speed epidermal wound healing, are currently in clinical trials. Here, we provide direct in vivo evidence that specific phosphorylation events on Cx43 change the physiological response during wound healing. Blocking phosphorylation, through mutation of serine residues in Cx43 at the protein kinase C (PKC) or casein kinase 1 (CK1) sites, significantly slowed the rate of wound closure in vivo and in vitro and resulted in a thicker epidermal layer after reepithelialization. Conversely, preventing Cx43 phosphorylation by mitogen-activated protein kinases (MAPKs) through mutation significantly increased the rate of wound closure in vivo Defects in migration, but not proliferation, in all mutants were partially rescued in vitro by changing serine residues to aspartic or glutamic acid . These data prove that specific Cx43 phosphorylation events play an important role at different stages of wound healing. Thus, a clear physiological understanding of the spatiotemporal regulation of kinase activation and consequent effects on gap junctions could lead to a more targeted approach to modulating Cx43 expression during wound healing., Competing Interests: Competing interestsThe authors declare no competing or financial interests., (© 2019. Published by The Company of Biologists Ltd.)

Published

2019

13. Cx43 phosphorylation-mediated effects on ERK and Akt protect against ischemia reperfusion injury and alter the stability of the stress-inducible protein NDRG1.

Author

Solan JL, Márquez-Rosado L, and Lampe PD

Subjects

Aging, Animals, Casein Kinase I metabolism, Connexin 43 genetics, Dogs, Gap Junctions metabolism, Madin Darby Canine Kidney Cells, Mice, Mice, Inbred C57BL, Mutagenesis, Myocardium metabolism, Phosphorylation drug effects, Protein Stability, Reperfusion Injury metabolism, Reperfusion Injury pathology, Substrate Specificity, Cell Cycle Proteins metabolism, Connexin 43 metabolism, Extracellular Signal-Regulated MAP Kinases metabolism, Intracellular Signaling Peptides and Proteins metabolism, Proto-Oncogene Proteins c-akt metabolism

Abstract

Gap junctions contain intercellular channels that enable intercellular communication of small molecules while also serving as a signaling scaffold. Connexins, the proteins that form gap junctions in vertebrates, are highly regulated and typically have short (<2 h) half-lives. Connexin43 (Cx43), the predominate connexin in the myocardium and epithelial tissues, is phosphorylated on more than a dozen serine residues and interacts with a variety of protein kinases. These interactions regulate Cx43 and gap junction formation and stability. Casein kinase 1 (CK1)-mediated phosphorylation of Cx43 promotes gap junction assembly. Using murine knock-in technology and quantitative PCR, immunoblotting, and immunoprecipitation assays, we show here that mutation of the CK1 phosphorylation sites in Cx43 reduces the levels of total Cx43 in the myocardium and increases Cx43 phosphorylation on sites phosphorylated by extracellular signal-regulated kinase (ERK). In aged myocardium, we found that, compared with WT Cx43, mutant Cx43 expression increases ERK activation, phosphorylation of Akt substrates, and protection from ischemia-induced injury. Our findings also uncovered that Cx43 interacts with the hypoxia-inducible protein N-Myc downstream-regulated gene 1 protein (NDRG1) and that Cx43 phosphorylation status controls this interaction and dramatically affects NDRG1 stability. We propose that, in addition to altering gap junction stability, Cx43 phosphorylation directly and dynamically regulates cellular signaling through ERK and Akt in response to ischemic injury. We conclude that gap junction-dependent NDRG1 regulation might explain some cellular responses to hypoxia., (© 2019 Solan et al.)

Published

2019

14. Spatio-temporal regulation of connexin43 phosphorylation and gap junction dynamics.

Author

Solan JL and Lampe PD

Subjects

Animals, Arrhythmias, Cardiac pathology, Biological Transport, Active, Gap Junctions pathology, Heart Failure pathology, Humans, Phosphorylation, Arrhythmias, Cardiac metabolism, Connexin 43 metabolism, Gap Junctions metabolism, Heart Failure metabolism, Second Messenger Systems

Abstract

Gap junctions are specialized membrane domains containing tens to thousands of intercellular channels. These channels permit exchange of small molecules (<1000Da) including ions, amino acids, nucleotides, metabolites and secondary messengers (e.g., calcium, glucose, cAMP, cGMP, IP 3 ) between cells. The common reductionist view of these structures is that they are composed entirely of integral membrane proteins encoded by the 21 member connexin human gene family. However, it is clear that the normal physiological function of this structure requires interaction and regulation by a variety of proteins, especially kinases. Phosphorylation is capable of directly modulating connexin channel function but the most dramatic effects on gap junction activity occur via the organization of the gap junction structures themselves. This is a direct result of the short half-life of the primary gap junction protein, connexin, which requires them to be constantly assembled, remodeled and turned over. The biological consequences of this remodeling are well illustrated during cardiac ischemia, a process wherein gap junctions are disassembled and remodeled resulting in arrhythmia and ultimately heart failure. This article is part of a Special Issue entitled: Gap Junction Proteins edited by Jean Claude Herve., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2018

15. Regulation of Cx37 channel and growth-suppressive properties by phosphorylation.

Author

Jacobsen NL, Pontifex TK, Li H, Solan JL, Lampe PD, Sorgen PL, and Burt JM

Subjects

Amino Acid Substitution, Animals, Cell Line, Tumor, Cell Survival physiology, Connexins genetics, Gap Junctions genetics, Mutation, Missense, Phosphorylation, Rats, Cell Cycle physiology, Connexins metabolism, Gap Junctions metabolism

Abstract

Growth suppression mediated by connexin 37 (Cx37; also known as GJA4) requires interaction between its C-terminus and functional pore-forming domain. Using rat insulinoma cells, we show that Cx37 induces cell death and cell cycle arrest, and slowed cell cycling. Whether differential phosphorylation might regulate intramolecular interactions, and consequently the growth-suppressive phenotype, is unknown. Protein kinase C inhibition increased the open state probability of low-conductance gap junction channels (GJChs) and reduced GJCh closed state probability. Substituting alanine at serine residues 275, 302 and 328 eliminated Cx37-induced cell death, supported proliferation and reduced the GJCh closed state probability. With additional alanine for serine substitutions at residues 285, 319, 321 and 325, Cx37-induced cell death was eliminated and the growth arrest period prolonged, and GJCh closed state probability was restored. With aspartate substitution at these seven sites, apoptosis was induced and the open state probability of large conductance GJChs (and hemichannels) was increased. These data suggest that differential phosphorylation of the C-terminus regulates channel conformation and, thereby, cell cycle progression and cell survival., Competing Interests: Competing interestsThe authors declare no competing or financial interests., (© 2017. Published by The Company of Biologists Ltd.)

Published

2017

16. Kinase programs spatiotemporally regulate gap junction assembly and disassembly: Effects on wound repair.

Author

Solan JL and Lampe PD

Subjects

Animals, Connexin 43 chemistry, Connexin 43 metabolism, Humans, Models, Biological, Phosphorylation, Gap Junctions metabolism, Protein Kinases metabolism, Wound Healing

Abstract

Gap junctions are highly ordered plasma membrane domains that are constantly assembled, remodeled and turned over due to the short half-life of connexins, the integral membrane proteins that form gap junctions. Connexin 43 (Cx43), by far the most widely expressed connexin, is phosphorylated at multiple serine residues in the cytoplasmic, C-terminal region allowing for exquisite cellular control over gap junctional communication. This is evident during epidermal wounding where spatiotemporal changes in connexin expression occur as cells are instructed whether to die, proliferate or migrate to promote repair. Early gap junctional communication is required for initiation of keratinocyte migration, but accelerated Cx43 turnover is also critical for proper wound healing at later stages. These events are controlled via a "kinase program" where sequential phosphorylation of Cx43 leads to reductions in Cx43's half-life and significant depletion of gap junctions from the plasma membrane within several hours. The complex regulation of gap junction assembly and turnover affords several steps where intervention might speed wound healing., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2016

17. Spatiotemporal proteomic analyses during pancreas cancer progression identifies serine/threonine stress kinase 4 (STK4) as a novel candidate biomarker for early stage disease.

Author

Mirus JE, Zhang Y, Hollingsworth MA, Solan JL, Lampe PD, and Hingorani SR

Subjects

Animals, Antibodies chemistry, Biomarkers, Tumor metabolism, Carcinoma, Pancreatic Ductal diagnosis, Carcinoma, Pancreatic Ductal metabolism, Carcinoma, Pancreatic Ductal pathology, Ceruletide, Diagnosis, Differential, Disease Models, Animal, Disease Progression, Early Diagnosis, Gene Expression Profiling, Humans, Mice, Molecular Sequence Annotation, Neoplasm Proteins metabolism, Pancreatic Neoplasms diagnosis, Pancreatic Neoplasms metabolism, Pancreatic Neoplasms pathology, Pancreatitis, Chronic chemically induced, Pancreatitis, Chronic diagnosis, Pancreatitis, Chronic metabolism, Protein Array Analysis, Protein Serine-Threonine Kinases metabolism, Proteome genetics, Proteome metabolism, Signal Transduction, Time Factors, Biomarkers, Tumor genetics, Carcinoma, Pancreatic Ductal genetics, Gene Expression Regulation, Neoplastic, Neoplasm Proteins genetics, Pancreatic Neoplasms genetics, Pancreatitis, Chronic genetics, Protein Serine-Threonine Kinases genetics

Abstract

Pancreas cancer, or pancreatic ductal adenocarcinoma, is the deadliest of solid tumors, with a five-year survival rate of <5%. Detection of resectable disease improves survival rates, but access to tissue and other biospecimens that could be used to develop early detection markers is confounded by the insidious nature of pancreas cancer. Mouse models that accurately recapitulate the human condition allow disease tracking from inception to invasion and can therefore be useful for studying early disease stages in which surgical resection is possible. Using a highly faithful mouse model of pancreas cancer in conjunction with a high-density antibody microarray containing ∼2500 antibodies, we interrogated the pancreatic tissue proteome at preinvasive and invasive stages of disease. The goal was to discover early stage tissue markers of pancreas cancer and follow them through histologically defined stages of disease using cohorts of mice lacking overt clinical signs and symptoms and those with end-stage metastatic disease, respectively. A panel of seven up-regulated proteins distinguishing pancreas cancer from normal pancreas was validated, and their levels were assessed in tissues collected at preinvasive, early invasive, and moribund stages of disease. Six of the seven markers also differentiated pancreas cancer from an experimental model of chronic pancreatitis. The levels of serine/threonine stress kinase 4 (STK4) increased between preinvasive and invasive stages, suggesting its potential as a tissue biomarker, and perhaps its involvement in progression from precursor pancreatic intraepithelial neoplasia to pancreatic ductal adenocarcinoma. Immunohistochemistry of STK4 at different stages of disease revealed a dynamic expression pattern further implicating it in early tumorigenic events. Immunohistochemistry of a panel of human pancreas cancers confirmed that STK4 levels were increased in tumor epithelia relative to normal tissue. Overall, this integrated approach yielded several tissue markers that could serve as signatures of disease stage, including early (resectable), and therefore clinically meaningful, stages., (© 2014 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2014

18. Specific Cx43 phosphorylation events regulate gap junction turnover in vivo.

Author

Solan JL and Lampe PD

Subjects

Animals, Cell Line, Connexin 43 genetics, Humans, Mitogen-Activated Protein Kinases metabolism, Phosphorylation, Zonula Occludens-1 Protein metabolism, Connexin 43 metabolism, Gap Junctions metabolism, Protein Processing, Post-Translational

Abstract

Gap junctions, composed of proteins from the connexin gene family, are highly dynamic structures that are regulated by kinase-mediated signaling pathways and interactions with other proteins. Phosphorylation of Connexin43 (Cx43) at different sites controls gap junction assembly, gap junction size and gap junction turnover. Here we present a model describing how Akt, mitogen activated protein kinase (MAPK) and src kinase coordinate to regulate rapid turnover of gap junctions. Specifically, Akt phosphorylates Cx43 at S373 eliminating interaction with zona occludens-1 (ZO-1) allowing gap junctions to enlarge. Then MAPK and src phosphorylate Cx43 to initiate turnover. We integrate published data with new data to test and refine this model. Finally, we propose that differential coordination of kinase activation and Cx43 phosphorylation controls the specific routes of disassembly, e.g., annular junction formation or gap junctions can potentially "unzip" and be internalized/endocytosed into the cell that produced each connexin., (Copyright © 2014 Federation of European Biochemical Societies. Published by Elsevier B.V. All rights reserved.)

Published

2014

19. Connexin43 phosphorylation in brain, cardiac, endothelial and epithelial tissues.

Author

Márquez-Rosado L, Solan JL, Dunn CA, Norris RP, and Lampe PD

Subjects

Animals, Connexin 43 metabolism, Genome, Human, Homeostasis, Humans, Models, Biological, Neoplasms metabolism, Phosphorylation, Signal Transduction, Tissue Distribution, Brain metabolism, Connexin 43 physiology, Endothelium metabolism, Epithelium metabolism, Gap Junctions physiology, Myocardium metabolism

Abstract

Gap junctions, composed of proteins from the connexin family, allow for intercellular communication between cells in essentially all tissues. There are 21 connexin genes in the human genome and different tissues express different connexin genes. Most connexins are known to be phosphoproteins. Phosphorylation can regulate connexin assembly into gap junctions, gap junction turnover and channel gating. Given the importance of gap junctions in development, proliferation and carcinogenesis, regulation of gap junction phosphorylation in response to wounding, hypoxia and other tissue insults is proving to be critical for cellular response and return to homeostasis. Connexin43 (Cx43) is the most widely and highly expressed gap junction protein, both in cell culture models and in humans, thus more research has been done on it and more reagents to it are available. In particular, antibodies that can report Cx43 phosphorylation status have been created allowing temporal examination of specific phosphorylation events in vivo. This review is focused on the use of these antibodies in tissue in situ, predominantly looking at Cx43 phosphorylation in brain, heart, endothelium and epithelium with reference to other connexins where data is available. These data allow us to begin to correlate specific phosphorylation events with changes in cell and tissue function. This article is part of a Special Issue entitled: The Communicating junctions, composition, structure and characteristics., (Copyright © 2011 Elsevier B.V. All rights reserved.)

Published

2012

20. CASK (LIN2) interacts with Cx43 in wounded skin and their coexpression affects cell migration.

Author

Márquez-Rosado L, Singh D, Rincón-Arano H, Solan JL, and Lampe PD

Subjects

Animals, Astrocytes metabolism, Base Sequence, Cell Adhesion Molecule-1, Cell Adhesion Molecules metabolism, Cell Line, Cell Movement physiology, Connexin 43 genetics, Dogs, Gene Knockdown Techniques, Guanylate Kinases antagonists & inhibitors, Guanylate Kinases genetics, Humans, Immunoglobulins metabolism, Male, Mice, Phosphorylation, RNA, Small Interfering genetics, Rats, Recombinant Proteins genetics, Recombinant Proteins metabolism, Skin cytology, Skin injuries, Skin metabolism, Transfection, Connexin 43 metabolism, Guanylate Kinases metabolism, Wound Healing physiology

Abstract

Vertebrate gap junctions are composed of proteins from the connexin family. Co-immunoprecipitation, in vitro binding and far western experiments demonstrate that mammalian CASK (also known as LIN2) directly interacts with Cx43. Immunoprecipitation studies indicate that the CASK mainly interacts with the hypophosphorylated form of Cx43. Functional co-regulation of these proteins was found in MDCK cells migrating into a scratch wound, where expression of either protein individually inhibits migration but their coexpression abrogates this inhibitory effect. Immunofluorescence shows colocalization of Cx43 and CASK in mouse brain astrocytes and in response to wounding in human foreskin. During wounding, CASK is mobilized to the plasma membrane where it colocalizes with Cx43 and CADM1 1 hour after skin explant wounding. Together, these studies indicate that CASK interaction with Cx43 occurs relatively early in the connexin life cycle and imply a plasma membrane targeting role for the interaction that apparently affects cellular processes including cellular migration and wound healing.

Published

2012

21. Trafficking and recycling of the connexin43 gap junction protein during mitosis.

Author

Boassa D, Solan JL, Papas A, Thornton P, Lampe PD, and Sosinsky GE

Subjects

Animals, Biological Transport, Cell Line, Cell Membrane metabolism, Connexin 43 chemistry, Connexin 43 genetics, Cytoplasmic Vesicles metabolism, Dogs, Fibroblasts cytology, Fluorescent Antibody Technique, Intracellular Space metabolism, Rats, Telophase, Connexin 43 metabolism, Mitosis physiology

Abstract

During the cell cycle, gap junction communication, morphology and distribution of connexin43 (Cx43)-containing structures change dramatically. As cells round up in mitosis, Cx43 labeling is mostly intracellular and intercellular coupling is reduced. We investigated Cx43 distributions during mitosis both in endogenous and exogenous expressing cells using optical pulse-chase labeling, correlated light and electron microscopy, immunocytochemistry and biochemical analysis. Time-lapse imaging of green fluorescent protein (GFP)/tetracysteine tagged Cx43 (Cx43-GFP-4C) expressing cells revealed an early disappearance of gap junctions, progressive accumulation of Cx43 in cytoplasmic structures, and an unexpected subset pool of protein concentrated in the plasma membrane surrounding the midbody region in telophase followed by rapid reappearance of punctate plaques upon mitotic exit. These distributions were also observed in immuno-labeled endogenous Cx43-expressing cells. Photo-oxidation of ReAsH-labeled Cx43-GFP-4C cells in telophase confirmed that Cx43 is distributed in the plasma membrane surrounding the midbody as apparent connexons and in cytoplasmic vesicles. We performed optical pulse-chase labeling and single label time-lapse imaging of synchronized cells stably expressing Cx43 with internal tetracysteine domains through mitosis. In late telophase, older Cx43 is segregated mainly to the plasma membrane while newer Cx43 is intracellular. This older population nucleates new gap junctions permitting rapid resumption of communication upon mitotic exit., (© 2010 John Wiley & Sons A/S.)

Published

2010

22. Connexin43 phosphorylation: structural changes and biological effects.

Author

Solan JL and Lampe PD

Subjects

Cell Cycle genetics, Cell Cycle physiology, Connexin 43 physiology, Gap Junctions metabolism, Gap Junctions physiology, Models, Biological, Phosphorylation physiology, Protein Processing, Post-Translational genetics, Protein Processing, Post-Translational physiology, Connexin 43 chemistry, Connexin 43 metabolism

Abstract

Vertebrate gap junctions, composed of proteins from the connexin gene family, play critical roles in embryonic development, co-ordinated contraction of excitable cells, tissue homoeostasis, normal cell growth and differentiation. Phosphorylation of connexin43, the most abundant and ubiquitously expressed connexin, has been implicated in the regulation of gap junctional communication at several stages of the connexin 'life cycle', including hemichannel oligomerization, export of the protein to the plasma membrane, hemichannel activity, gap junction assembly, gap junction channel gating and connexin degradation. Consistent with a short (1-5 h) protein half-life, connexin43 phosphorylation is dynamic and changes in response to activation of many different kinases. The present review assesses our current understanding of the effects of phosphorylation on connexin43 structure and function that in turn regulate gap junction biology, with an emphasis on events occurring in heart and skin.

Published

2009

23. Connexin 43 in LA-25 cells with active v-src is phosphorylated on Y247, Y265, S262, S279/282, and S368 via multiple signaling pathways.

Author

Solan JL and Lampe PD

Subjects

Amino Acid Sequence, Animals, Cell Line, Connexin 43 genetics, Dogs, Gap Junctions metabolism, Humans, Molecular Sequence Data, Phosphorylation, Rats, Serine genetics, Tyrosine genetics, Connexin 43 metabolism, Oncogene Protein pp60(v-src) physiology, Serine metabolism, Signal Transduction physiology, Tyrosine metabolism

Abstract

Modulation of gap junction structures and gap junctional communication is important in maintaining tissue homeostasis and can be controlled via phosphorylation of connexin 43 (Cx43) through several different signaling pathways. Transformation of cells by v-src has been shown to down-regulate gap junction communication coincident with an increase in tyrosine phosphorylation on Cx43. Activation of mitogen-activated protein kinase (MAPK) and protein kinase C (PKC) also lead to down-regulation via phosphorylation on specific serine residues. Using phosphospecific anti-Cx43 antibodies generated by the authors' laboratory to specific tyrosines (src substrates) and serine residues (MAPK and PKC substrates) to probe LA-25 cells (which express temperature-sensitive v-src), the authors show that distinct tyrosine and serines residues are phosphorylated in response to v-src activity. They show that tyrosine phosphorylation appears to occur predominantly in gap junction plaques when src is active. In addition, src activation led to increased phosphorylation of apparent MAPK and PKC sites in Cx43. These results indicate all three signaling pathways could contribute to gap junction down-regulation during src transformation in LA-25 cells.

Published

2008

24. Phosphorylation at S365 is a gatekeeper event that changes the structure of Cx43 and prevents down-regulation by PKC.

Author

Solan JL, Marquez-Rosado L, Sorgen PL, Thornton PJ, Gafken PR, and Lampe PD

Subjects

Amino Acid Substitution, Animals, Blotting, Western, Cell Line, Connexin 43 chemistry, Connexin 43 genetics, Connexins chemistry, Connexins genetics, Dogs, Fluorescent Antibody Technique, Hypoxia metabolism, Mice, Myocardium metabolism, Nuclear Magnetic Resonance, Biomolecular, Phosphorylation, Protein Isoforms chemistry, Protein Isoforms metabolism, Protein Structure, Tertiary, Rats, Serine metabolism, Connexin 43 metabolism, Connexins metabolism, Down-Regulation, Protein Kinase C metabolism

Abstract

Phosphorylation at unspecified sites is known to regulate the life cycle (assembly, gating, and turnover) of the gap junction protein, Cx43. In this paper, we show that Cx43 is phosphorylated on S365 in cultured cells and heart tissue. Nuclear magnetic resonance structural studies of the C-terminal region of Cx43 with an S365D mutation indicate that it forms a different stable conformation than unphosphorylated wild-type Cx43. Immunolabeling with an antibody specific for Cx43 phosphorylated at S365 shows staining on gap junction structures in heart tissue that is lost upon hypoxia when Cx43 is no longer specifically localized to the intercalated disk. Efficient phosphorylation at S368, an important Cx43 channel regulatory event that increases during ischemia or PKC activation, depends on S365 being unphosphorylated. Thus, phosphorylation at S365 can serve a "gatekeeper" function that may represent a mechanism to protect cells from ischemia and phorbol ester-induced down-regulation of channel conductance.

Published

2007

25. The C-terminus of connexin43 adopts different conformations in the Golgi and gap junction as detected with structure-specific antibodies.

Author

Sosinsky GE, Solan JL, Gaietta GM, Ngan L, Lee GJ, Mackey MR, and Lampe PD

Subjects

Animals, Cell Line, Connexin 43 genetics, Connexin 43 immunology, Dogs, Electrophoresis, Polyacrylamide Gel, Immunoprecipitation, Microscopy, Confocal, Microscopy, Fluorescence, Mutagenesis, Site-Directed, Phosphorylation, Protein Conformation, Rats, Antibodies immunology, Connexin 43 chemistry, Gap Junctions chemistry, Golgi Apparatus chemistry

Abstract

The C-terminus of the most abundant and best-studied gap-junction protein, connexin43, contains multiple phosphorylation sites and protein-binding domains that are involved in regulation of connexin trafficking and channel gating. It is well-documented that SDS/PAGE of NRK (normal rat kidney) cell lysates reveals at least three connexin43-specific bands (P0, P1 and P2). P1 and P2 are phosphorylated on multiple, unidentified serine residues and are found primarily in gap-junction plaques. In the present study we prepared monoclonal antibodies against a peptide representing the last 23 residues at the C-terminus of connexin43. Immunofluorescence studies showed that one antibody (designated CT1) bound primarily to connexin43 present in the Golgi apparatus, whereas the other antibody (designated IF1) labelled predominately connexin43 present in gap junctions. CT1 immunoprecipitates predominantly the P0 form whereas IF1 recognized all three bands. Peptide mapping, mutational analysis and protein-protein interaction experiments revealed that unphosphorylated Ser364 and/or Ser365 are critical for CT1 binding. The IF1 paratope binds to residues Pro375-Asp379 and requires Pro375 and Pro377. These proline residues are also necessary for ZO-1 interaction. These studies indicate that the conformation of Ser364/Ser365 is important for intracellular localization, whereas the tertiary structure of Pro375-Asp379 is essential in targeting and regulation of gap junctional connexin43.

Published

2007

26. Key connexin 43 phosphorylation events regulate the gap junction life cycle.

Author

Solan JL and Lampe PD

Subjects

Animals, CHO Cells, Cells, Cultured, Cricetinae, Cricetulus, Dogs, Enzyme Activation drug effects, Fluorescent Antibody Technique, HeLa Cells, Humans, Immunoblotting, Kidney cytology, Phosphorylation, Protein Isoforms, Protein Kinase C metabolism, Cell Communication, Connexin 43 metabolism, Gap Junctions metabolism

Abstract

Connexin 43 (Cx43), the most widely expressed and abundant vertebrate gap junction protein, is phosphorylated at multiple different serine residues during its life cycle. Cx43 is phosphorylated soon after synthesis and phosphorylation changes as it traffics through the endoplasmic reticulum and Golgi to the plasma membrane, ultimately forming a gap junction structure. The electrophoretic mobility of Cx43 changes as the protein proceeds through its life cycle, with prominent bands often labeled P0, P1 and P2. Many reports have indicated changes in "phosphorylation" based on these mobility shifts and others that occur in response to growth factors or other biological effectors. Here, we indicate how phosphospecific and epitope-specific antibodies can be utilized to show when and where certain phosphorylation events occur during the Cx43 life cycle. These reagents show that phosphorylation at S364 and/or S365 is involved in forming the P1 isoform, an event that apparently regulates trafficking to or within the plasma membrane. Phosphorylation at S325, S328 and/or S330 is necessary to form a P2 isoform; and this phosphorylation event is present only in gap junctions. Treatment with protein kinase C activators led to phosphorylation at S368, S279/S282 and S262 with a shift in mobility in CHO, but not MDCK, cells. The shift was dependent on mitogen-activated protein kinase activity but not phosphorylation at S279/S282. However, phosphorylation at S262 could explain the shift. By defining these phosphorylation events, we have begun to sort out the critical signaling pathways that regulate gap junction function.

Published

2007

27. Connexin 43 interacts with zona occludens-1 and -2 proteins in a cell cycle stage-specific manner.

Author

Singh D, Solan JL, Taffet SM, Javier R, and Lampe PD

Subjects

Animals, Blotting, Western, Cell Cycle, Cell Line, Cell Membrane metabolism, Chromatography, Connexin 43 chemistry, Cytoplasm metabolism, Detergents pharmacology, Epithelial Cells cytology, Gap Junctions, Glutathione Transferase metabolism, Immunoblotting, Immunoprecipitation, Kidney metabolism, Mass Spectrometry, Microscopy, Confocal, Microscopy, Fluorescence, Octoxynol pharmacology, Plasmids metabolism, Protein Binding, Protein Structure, Tertiary, Rats, Recombinant Fusion Proteins chemistry, S Phase, Trypsin chemistry, Zonula Occludens-1 Protein, Zonula Occludens-2 Protein, Connexin 43 metabolism, Membrane Proteins metabolism, Phosphoproteins metabolism

Abstract

Gap junction channels play an important role in cell growth control, secretion and embryonic development. Gap junctional communication and channel assembly can be regulated by protein-protein interaction with kinases and phosphatases. We have utilized tandem mass spectrometry (MS/MS) sequence analysis as a screen to identify proteins from cell lysates that interact with the C-terminal cytoplasmic region of connexin 43 (Cx43). MS/MS analysis of tryptic fragments yielded several proteins including zona occludens-1 (ZO-1), a structural protein previously identified to interact with Cx43, and ZO-2, a potential novel interacting partner. We confirmed the interaction of ZO-2 with Cx43 by using a combination of fusion protein "pull down," co-immunoprecipitation, and co-localization experiments. We show that the C-terminal region of Cx43 is necessary for interaction with the PDZ2 domain of ZO-2. Far Western analysis revealed that ZO-2 can directly bind to Cx43 independent of other interacting partners. Immunofluorescence studies indicate that both ZO-1 and ZO-2 can co-localize with Cx43 within the plasma membrane at apparent gap junctional structures. We examined Cx43 interaction with ZO-1 and ZO-2 at different stages of the cell cycle and found that Cx43 had a strong preference for interaction with ZO-1 during G0, whereas ZO-2 interaction occurred approximately equally during G0 and S phases. Since essentially all of the Cx43 in G0 cells is assembled into Triton X-100-resistant junctions, Cx43-ZO-1 interaction may contribute to their stability.

Published

2005

28. Connexin phosphorylation as a regulatory event linked to gap junction channel assembly.

Author

Solan JL and Lampe PD

Subjects

Amino Acid Sequence, Animals, Casein Kinase I metabolism, Cell Communication physiology, Cell Cycle, Connexin 43 metabolism, Cyclic AMP physiology, Humans, Molecular Sequence Data, Protein Kinase C metabolism, Connexins metabolism, Gap Junctions metabolism, Ion Channels biosynthesis

Abstract

Gap junctions, composed of proteins from the connexin family, allow for intercellular communication between cells and are important in development and maintenance of cell homeostasis. Phosphorylation has been implicated in the regulation of gap junctional communication at several stages of the cell cycle and the connexin "lifecycle", such as trafficking, assembly/disassembly, degradation, as well as in the gating of "hemi" channels or intact gap junction channels. This review focuses on how phosphorylation can regulate the early stages of the connexin life cycle through assembly of functional gap junctional channels. The availability of sequences from the human genome databases has indicated that the number of connexins in the gene family is approximately 20, but we know mostly about how connexin43 (Cx43) is regulated. Recent technologies and investigations of interacting proteins have shown that activation of several kinases including protein kinase A, protein kinase C (PKC), p34(cdc2)/cyclin B kinase, casein kinase 1 (CK1), mitogen-activated protein kinase (MAPK) and pp60(src) kinase can lead to phosphorylation of the majority of the 21 serine and two of the tyrosine residues in the C-terminal region of Cx43. While many studies have correlated changes in kinase activity with changes in gap junctional communication, further research is needed to directly link specific phosphorylation events with changes in connexin oligomerization and gap junction assembly.

Published

2005

29. Connexin43 phosphorylation at S368 is acute during S and G2/M and in response to protein kinase C activation.

Author

Solan JL, Fry MD, TenBroek EM, and Lampe PD

Subjects

Animals, Antibody Specificity, Carcinogens pharmacology, Cell Membrane metabolism, Cells, Cultured, Connexin 43 immunology, Cytoplasm metabolism, Enzyme Activation drug effects, Gap Junctions metabolism, Kidney cytology, Phosphorylation, Rats, Serine metabolism, Tetradecanoylphorbol Acetate pharmacology, Connexin 43 metabolism, G2 Phase physiology, Mitosis physiology, Protein Kinase C metabolism, S Phase physiology

Abstract

Phorbol esters such as 12-O-tetradeconylphorbol-13-acetate (TPA) activate protein kinase C, increase Connexin43 (Cx43) phosphorylation, and decrease cell-cell communication via gap junctions in many cell types. Previous work has implicated protein kinase C (PKC) in the direct phosphorylation of Cx43 at S368, which results in a change in single channel behavior that contributes to a decrease in intercellular communication. We have examined Cx43 phosphorylation in several cell lines with an antibody specific for phosphorylated S368. We show that this antibody detects Cx43 only when it is phosphorylated at S368 and, consistent with previous results, TPA treatment causes a dramatic increase in phosphorylation at S368. However, in some cell types, the increased phosphorylation at S368 did not cause a detectable shift in migration as compared with the nonphosphorylated Cx43. Immunofluorescence showed increased S368 immunolabeling in cytoplasmic and plasma membrane structures in response to TPA. Immunoblot analysis of synchronized cells showed increased phosphorylation at S368 during S and G2/M phases of the cell cycle. S-phase cells contained more total Cx43 but assembled fewer functional gap junctional channels than G0-phase cells. Since M-phase cells also communicate poorly and contain few assembled gap junctions, phosphorylation at S368 appears to be negatively correlated with gap junction assembly. Thus, both gap junctional communication and S368 phosphorylation change during S phase and G2/M, implying that phosphorylation at S368 might play a role in key cell-cycle events.

Published

2003

30. Ser364 of connexin43 and the upregulation of gap junction assembly by cAMP.

Author

TenBroek EM, Lampe PD, Solan JL, Reynhout JK, and Johnson RG

Subjects

Animals, Cell Line, Connexin 43 genetics, Fibroblasts ultrastructure, G1 Phase, Green Fluorescent Proteins, Kinetics, Luminescent Proteins metabolism, Mice, Phosphorylation, Recombinant Fusion Proteins metabolism, Recombinant Proteins metabolism, Transfection, Connexin 43 metabolism, Gap Junctions physiology, Phosphoserine metabolism, Serine

Abstract

The assembly of gap junctions (GJs) is a process coordinated by growth factors, kinases, and other signaling molecules. GJ assembly can be enhanced via the elevation of cAMP and subsequent stimulation of connexon trafficking to the plasma membrane. To study the positive regulation of GJ assembly, fibroblasts derived from connexin (Cx)43 knockout (KO) and wild-type (WT) mice were transfected with WT Cx43 (WTCx43) or mutant Cx43. GJ assembly between untransfected WT fibroblasts or stably transfected WTCx43/KO fibroblasts was increased two- to fivefold by 8Br-cAMP, and this increase could be blocked by inhibition of cAMP-dependent protein kinase (PKA) or truncation of the Cx43 COOH terminus (CT). Although serine 364 (S364) of the Cx43 CT was determined to be a major site of phosphorylation, the molar ratio of Cx43 phosphorylation was not increased by 8Br-cAMP. Importantly, GJ assembly between either S364ECx43/KO or S364ECx43/WT fibroblasts was stimulated by 8Br-cAMP, but that between S364ACx43/KO or S364PCx43/KO fibroblasts was not stimulated, indicating that phosphorylation or a negative charge at S364 is required for enhancement of GJ assembly by cAMP. Furthermore, GJ assembly between S364ACx43/WT fibroblasts could be stimulated by 8Br-cAMP, but could not be between S364PCx43/WT fibroblasts. Thus, S364PCx43 interferes with enhanced GJ assembly when coexpressed with WTCx43.

Published

2001

31. The regulatory role of the C-terminal domain of connexin43.

Author

Shin JL, Solan JL, and Lampe PD

Subjects

Animals, Anti-Bacterial Agents metabolism, Cell Communication physiology, Cell Line, Connexin 43 genetics, Doxycycline metabolism, Humans, Phosphorylation, Promoter Regions, Genetic, Protein Structure, Tertiary, Rats, Recombinant Fusion Proteins genetics, Tetradecanoylphorbol Acetate metabolism, Connexin 43 metabolism, Gene Expression Regulation, Recombinant Fusion Proteins metabolism

Abstract

The C-terminal (CT) domain of connexin43 (Cx43) is thought to be important in the control of gap junction function via: a.) CT phosphorylation-dependent control of gap junction assembly and gating, b.) interactions of CT with key regulatory binding partners. To more closely examine CT-dependent regulation, we have expressed a hemagglutinin-Cx43CT (amino acids 235-382) fusion protein in Normal Rat Kidney (NRK) cells under a tetracycline-responsive inducible promoter. Western blot analysis shows that Cx43CT expression is markedly induced by at least 48 h oftreatment with the tetracycline analogue, doxycycline. Furthermore, Cx43CT is modified within the cell, as several treatments/conditions that increase endogenous Cx43 phosphorylation induced a mobility shift in Cx43CT. Treatment with kinase activators, including epidermal growth factor (EGF) and the tumor promoting phorbol ester 12-O-tetradecanylphorbol-13-acetate (TPA), caused a shift in the mobility of the Cx43CT in a manner consistent with the mobility shift observed upon increased phosphorylation of endogenous Cx43. Similarly, Cx43CT in mitotic cells is extensively shifted, consistent with reports which show that Cx43 is phosphorylated to a unique phosphoisoform in mitotic cells. These results indicate that the Cx43CT can interact with at least some of the kinases that phosphorylate endogenous Cx43 in cells and possibly modulate the effects of kinase activation on gap junctional communication.

Published

2001

32. Analysis of connexin phosphorylation sites.

Author

Cooper CD, Solan JL, Dolejsi MK, and Lampe PD

Subjects

Amino Acid Sequence, Animals, Automation, Cell Communication, Cell Culture Techniques methods, Cell Line, Chromatography, High Pressure Liquid, Connexin 43 genetics, Insecta, Kidney, Mass Spectrometry, Molecular Sequence Data, Peptide Fragments chemistry, Phosphopeptides chemistry, Phosphorylation, Rats, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Transfection, Connexin 43 chemistry, Connexin 43 metabolism, Gap Junctions physiology

Abstract

Most connexins, the proteins that form gap junction channels, are phosphoproteins. Connexin phosphorylation has been thought to regulate gap junctional protein trafficking, gap junction assembly, channel gating, and turnover. Connexin phosphorylation has been investigated in a variety of ways. Some connexins show mobility shifts in sodium dodecyl sulfate-polyacrylamide gel electrophoresis on phosphorylation. Kinase modulators can change the level of connexin phosphorylation and affect gap junctional communication levels. Metabolic labeling of cultured cells has allowed both phosphoamino acid identification and generation of phosphotryptic peptide maps. However, identification of the location of phosphorylated residues within the connexin sequence has required either targeted peptide synthesis, in vitro phosphorylation of known sites, and two-dimensional comigration studies or liquid chromatographic separation and N-terminal sequencing of peptides. In addition to these conventional methods, we discuss new applications of mass spectrometry to the identification of phosphorylated peptides and the specific residues phosphorylated within the connexin-derived peptide., (Copyright 2000 Academic Press.)

Published

2000

33. Trafficking, assembly, and function of a connexin43-green fluorescent protein chimera in live mammalian cells.

Author

Jordan K, Solan JL, Dominguez M, Sia M, Hand A, Lampe PD, and Laird DW

Subjects

Animals, Biological Transport, Cell Line, Cell Membrane metabolism, Dogs, Gap Junctions ultrastructure, Green Fluorescent Proteins, Humans, Image Enhancement, Luminescent Proteins analysis, Mammals metabolism, Microinjections, Microscopy, Confocal, Octoxynol chemistry, Rats, Recombinant Fusion Proteins analysis, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins metabolism, Time Factors, Connexin 43 genetics, Connexin 43 metabolism, Gap Junctions metabolism, Luminescent Proteins genetics, Luminescent Proteins metabolism

Abstract

To examine the trafficking, assembly, and turnover of connexin43 (Cx43) in living cells, we used an enhanced red-shifted mutant of green fluorescent protein (GFP) to construct a Cx43-GFP chimera. When cDNA encoding Cx43-GFP was transfected into communication-competent normal rat kidney cells, Cx43-negative Madin-Darby canine kidney (MDCK) cells, or communication-deficient Neuro2A or HeLa cells, the fusion protein of predicted length was expressed, transported, and assembled into gap junctions that exhibited the classical pentalaminar profile. Dye transfer studies showed that Cx43-GFP formed functional gap junction channels when transfected into otherwise communication-deficient HeLa or Neuro2A cells. Live imaging of Cx43-GFP in MDCK cells revealed that many gap junction plaques remained relatively immobile, whereas others coalesced laterally within the plasma membrane. Time-lapse imaging of live MDCK cells also revealed that Cx43-GFP was transported via highly mobile transport intermediates that could be divided into two size classes of <0.5 microm and 0.5-1.5 microm. In some cases, the larger intracellular Cx43-GFP transport intermediates were observed to form from the internalization of gap junctions, whereas the smaller transport intermediates may represent other routes of trafficking to or from the plasma membrane. The localization of Cx43-GFP in two transport compartments suggests that the dynamic formation and turnover of connexins may involve at least two distinct pathways.

Published

1999

34. Expression of the nucleoside triphosphate pyrophosphohydrolase PC-1 is induced by basic fibroblast growth factor (bFGF) and modulated by activation of the protein kinase A and C pathways in osteoblast-like osteosarcoma cells.

Author

Solan JL, Deftos LJ, Goding JW, and Terkeltaub RA

Subjects

Enzyme Activation, Fibroblast Growth Factor 1 pharmacology, Humans, Osteosarcoma, Tumor Cells, Cultured, Cyclic AMP-Dependent Protein Kinases metabolism, Fibroblast Growth Factor 2 pharmacology, Osteoblasts drug effects, Protein Kinase C metabolism, Pyrophosphatases biosynthesis

Abstract

The closely related cytokines bFGF and aFGF regulate the function of bone cells and mineralization. Osteoblasts express PPi-generating nucleoside triphosphate pyrophosphohydrolase (NTPPPH)/nucleotide phosphodiesterase I activity. bFGF and aFGF (10 ng/ml) up-regulated NTPPPH in human SaOS-2 and U2OS osteosarcoma cells, which express osteoblast-like features in culture. The induction was selective as alkaline phosphatase activity was down-regulated and specific as insulin-like growth factor-1 (IGF-1) and interleukin-1 beta (IL-1 beta) were not active. Furthermore, IL-1 beta but not IGF-1 inhibited bFGF-induced up-regulation of NTPPPH. The induced NTPPPH remained predominantly associated with cells. bFGF can induce signaling through pathways including protein kinase A (PKA) and protein kinase C (PKC)-mediated transduction. An activator of the PKA pathway (8-bromo cyclic adenosine monophosphate [cAMP]) induced NTPPPH. Furthermore, pretreatment with the PKC activator phorbol myristate acetate (PMA) (80 nM) markedly increased subsequent NTPPPH induction by both bFGF and cAMP. The PMA effect was associated with morphologic changes characterized by long, thin intercellular extensions. PKC desensitization also potentially contributed to this effect because the PKC inhibitors staurosporine and H-7 enhanced bFGF-induced and cAMP-induced NTPPPH expression in the absence of morphologic changes. We observed that bFGF induced expression of PC-1, a member of the NTPPPH gene family. The majority of NTPPPH activity was depleted by immunoadsorption using a monoclonal antibody to native human PC-1. bFGF- and aFGF-induced production of PC-1/NTPPPH in osteoblastoid cells may contribute to the effects of FGFs on bone metabolism.

Published

1996

35. A METHOD FOR SEPARATING SATURATED FATTY ACID ESTERS FROM UNSATURATED ESTERS FOR GAS CHROMATOGRAPHIC ANALYSIS.

Author

KOEHLER WR, SOLAN JL, and HAMMOND HT

Subjects

Rats, Bromine, Chromatography, Esters, Fats, Unsaturated, Fatty Acids, Fatty Acids, Essential, Linoleic Acid, Oleic Acid, Oleic Acids, Palmitic Acid, Research, Skin, Stearic Acids

Published

1964