Your search keyword '"Bouley, Donna M."' showing total 19 results

1. Progressive ataxia, myoclonic epilepsy and cerebellar apoptosis in cystatin B-deficient mice.

Author

Pennacchio, Len A., Bouley, Donna M., Higgins, Kay M., Scott, Matthew P., Noebels, Jeffrey L., and Myers, Richard M.

Subjects

*NEUROLOGICAL disorders, *ATAXIA, *EPILEPSY, *APOPTOSIS

Abstract

Loss-of-function mutations in the gene (CSTB) encoding human cystatin B, a widely expressed cysteine protease inhibitor, are responsible for a severe neurological disorder known as Unverricht-Lundborg disease (EPM1). The primary cellular events and mechanisms underlying the disease are unknown. We found that mice lacking cystatin B develop myoclonic seizures and ataxia, similar to symptoms seen in the human disease. The principal cytopathology appears to be a loss of cerebellar granule cells, which frequently display condensed nuclei, fragmented DNA and other cellular changes characteristic of apoptosis. This mouse model of EPM1 provides evidence that cystatin B, a non-caspase cysteine protease inhibitor, has a role in preventing cerebellar apoptosis. [ABSTRACT FROM AUTHOR]

Published

1998

2. Role of disease-associated tolerance in infectious superspreaders.

Author

Gopinatha, Smita, Lichtman, Joshua S., Bouley, Donna M., Elias, Joshua E., and Monack, Denise M.

Subjects

*HETEROGENEITY, *ECOLOGICAL heterogeneity, *ANTIBIOTICS, *CYTOKINES, *MYELOID leukemia

Abstract

Natural populations show striking heterogeneity in their ability to transmit disease. For example, a minority of infected individuals known as superspreaders carries out the majority of pathogen transmission events. In a mouse model of Salmonella infection, a subset of infected hosts becomes superspreaders, shedding high levels of bacteria (>108 cfu per g of feces) but remain asymptomatic with a dampened systemic immune state. Here we show that superspreader hosts remain asymptomatic when they are treated with oral antibiotics. In contrast, nonsuperspreader Salmonella-infected hosts that are treated with oral antibiotics rapidly shed superspreader levels of the pathogen but display signs of morbidity. This morbidity is linked to an increase in inflammatory myeloid cells in the spleen followed by increased production of acute-phase proteins and proinflammatory cytokines. The degree of colonic inflammation is similar in antibiotic-treated superspreader and nonsuperspreader hosts, indicating that the superspreader hosts are tolerant of antibiotic-mediated perturbations in the intestinal tract. Importantly, neutralization of acute-phase proinflammatory cytokines in antibiotic-induced superspreaders suppresses the expansion of inflammatory myeloid cells and reduces morbidity. We describe a unique disease-associated tolerance to oral antibiotics in superspreaders that facilitates continued transmission of the pathogen. [ABSTRACT FROM AUTHOR]

Published

2014

3. Characterization of a novel anthropomorphic plastinated lung phantom.

Author

Sungwon Yoon, Henry, Robert W., Bouley, Donna M., Bennett, N. Robert, and Fahrig, Rebecca

Subjects

*IMAGING phantoms, *ANTHROPOMETRY, *MEDICAL imaging systems, *ALGORITHMS, *PLASTINATION

Abstract

Phantoms are widely used during the development of new imaging systems and algorithms. For development and optimization of new imaging systems such as tomosynthesis, where conventional image quality metrics may not be applicable, a realistic phantom that can be used across imaging systems is desirable. A novel anthropomorphic lung phantom was developed by plastination of an actual pig lung. The plastinated phantom is characterized and compared with reference to in vivo images of the same tissue prior to plastination using high resolution 3D CT. The phantom is stable over time and preserves the anatomical features and relative locations of the in vivo sample. The volumes for different tissue types in the phantom are comparable to the in vivo counterparts, and CT numbers for different tissue types fall within a clinically useful range. Based on the measured CT numbers, the phantom cardiac tissue experienced a 92% decrease in bulk density and the phantom pulmonary tissue experienced a 78% decrease in bulk density compared to their in vivo counterparts. By-products in the phantom from the room temperature vulcanizing silicone and plastination process are also identified. A second generation phantom, which eliminates most of the by-products, is presented. Such anthropomorphic phantoms can be used to evaluate a wide range of novel imaging systems. [ABSTRACT FROM AUTHOR]

Published

2008

4. Neonatal Lethality of LGR5 Null Mice Is Associated with Ankyloglossia and Gastrointestinal Distension.

Author

Morita, Hiroki, Mazerbourg, Sabine, Bouley, Donna M., Ching-Wei Luo, Kawamura, Kazuhiro, Kuwabara, Yoshimitsu, Baribault, Helene, Hui Tian, and Hsueh, Aaron J. W.

Subjects

*G proteins, *MEMBRANE proteins, *GASTROINTESTINAL system, *ANKYLOGLOSSIA, *HUMAN embryos

Abstract

The physiological role of an orphan G protein-coupled receptor, LGR5, was investigated by targeted deletion of this seven-transmembrane protein containing a large N-terminal extracellular domain with leucine-rich repeats. LGR5 null mice exhibited 100% neonatal lethality characterized by gastrointestinal tract dilation with air and an absence of milk in the stomach. Gross and histological examination revealed fusion of the tongue to the floor of oral cavity in the mutant newborns and immunostaining of LGR5 expression in the epithelium of the tongue and in the mandible of the wild-type embryos. The observed ankyloglossia phenotype provides a model for understanding the genetic basis of this craniofacial defect in humans and an opportunity to elucidate the physiological role of the LGR5 signaling system during embryonic development. [ABSTRACT FROM AUTHOR]

Published

2004

5. A biochemical function for attractin in agouti-induced pigmentation and obesity.

Author

He, Lin, Gunn, Teresa M., Bouley, Donna M., Lu, Xin-Yun, Watson, Stanley J., Schlossman, Stuart F., Duke-Cohan, Jonathan S., and Barsh, Gregory S.

Subjects

*AGOUTI (Genus), *PROTEINS, *BIOCHEMISTRY

Abstract

Agouti protein, a paracrine signaling molecule normally limited to skin, is ectopically expressed in lethal yellow (Ay) mice, and causes obesity by mimicking agouti-related protein (Agrp), found primarily in the hypothalamus. Mouse attractin (Atrn) is a widely expressed transmembrane protein whose loss of function in mahogany (Atrnmg-3J/Atrnmg-3J) mutant mice blocks the pleiotropic effects of Ay. Here we demonstrate in transgenic, biochemical and genetic-interaction experiments that attractin is a low-affinity receptor for agouti protein, but not Agrp, in vitro and in vivo. Additional histopathologic abnormalities in Atrnmg-3J/Atrnmg-3J mice and cross-species genomic comparisons indicate that Atrn has multiple functions distinct from both a physiologic and an evolutionary perspective. [ABSTRACT FROM AUTHOR]

Published

2001

6. The glucosyltransferase activity of C. difficile Toxin B is required for disease pathogenesis.

Author

Bilverstone, Terry W., Garland, Megan, Cave, Rory J., Kelly, Michelle L., Tholen, Martina, Bouley, Donna M., Kaye, Philip, Minton, Nigel P., Bogyo, Matthew, Kuehne, Sarah A., and Melnyk, Roman A.

Subjects

*PATHOLOGY, *CLOSTRIDIOIDES difficile, *TOXINS, *SYMPTOMS, *HAMSTERS, *DISEASES, *MOUSE diseases

Abstract

Enzymatic inactivation of Rho-family GTPases by the glucosyltransferase domain of Clostridioides difficile Toxin B (TcdB) gives rise to various pathogenic effects in cells that are classically thought to be responsible for the disease symptoms associated with C. difficile infection (CDI). Recent in vitro studies have shown that TcdB can, under certain circumstances, induce cellular toxicities that are independent of glucosyltransferase (GT) activity, calling into question the precise role of GT activity. Here, to establish the importance of GT activity in CDI disease pathogenesis, we generated the first described mutant strain of C. difficile producing glucosyltransferase-defective (GT-defective) toxin. Using allelic exchange (AE) technology, we first deleted tcdA in C. difficile 630Δerm and subsequently introduced a deactivating D270N substitution in the GT domain of TcdB. To examine the role of GT activity in vivo, we tested each strain in two different animal models of CDI pathogenesis. In the non-lethal murine model of infection, the GT-defective mutant induced minimal pathology in host tissues as compared to the profound caecal inflammation seen in the wild-type and 630ΔermΔtcdA (ΔtcdA) strains. In the more sensitive hamster model of CDI, whereas hamsters in the wild-type or ΔtcdA groups succumbed to fulminant infection within 4 days, all hamsters infected with the GT-defective mutant survived the 10-day infection period without primary symptoms of CDI or evidence of caecal inflammation. These data demonstrate that GT activity is indispensable for disease pathogenesis and reaffirm its central role in disease and its importance as a therapeutic target for small-molecule inhibition. Author summary: Novel non-antibiotic therapies are required for the treatment of Clostridioides difficile infection (CDI). An emerging class of promising therapeutics for CDI are antivirulence agents that block the actions of C. difficile Toxin B (TcdB), the primary determinant of virulence. In order to develop such treatments, molecular targets and mechanisms must be identified and validated. Historically the glucosyltransferase domain (GTD) represented an ideal target owing to its perceived importance for disease pathogenesis. However, studies capitalizing on recent advances in recombinant TcdB production have unveiled GTD-independent mechanisms of toxicity when applied at high concentrations in vitro, thus questioning the role of the GTD. Here we generate the first-reported mutant strain of C. difficile expressing glucosyltransferase-defective TcdB. Application thereof demonstrates that the GTD is essential for disease in mice and hamsters, thus reoffering the GTD as an ideal candidate for small-molecule inhibitor (SMI) development. [ABSTRACT FROM AUTHOR]

Published

2020

7. Toxoplasma gondii infection triggers chronic cachexia and sustained commensal dysbiosis in mice.

Author

Hatter, Jessica A., Kouche, Yue Moi, Melchor, Stephanie J., Ng, Katherine, Bouley, Donna M., Boothroyd, John C., and Ewald, Sarah E.

Subjects

*TOXOPLASMA gondii, *CACHEXIA, *LEAN body mass, *CHRONIC diseases, *PREDATION, *DISEASE progression

Abstract

Toxoplasma gondii is a protozoan parasite with a predation-mediated transmission cycle between rodents and felines. Intermediate hosts acquire Toxoplasma by eating parasite cysts which invade the small intestine, disseminate systemically and finally establish host life-long chronic infection in brain and muscles. Here we show that Toxoplasma infection can trigger a severe form of sustained cachexia: a disease of progressive lean weight loss that is a causal predictor of mortality in cancer, chronic disease and many infections. Toxoplasma cachexia is characterized by acute anorexia, systemic inflammation and loss of 20% body mass. Although mice recover from symptoms of peak sickness, they fail to regain muscle mass or visceral adipose depots. We asked whether the damage to the intestinal microenvironment observed at acute time points was sustained in chronic infection and could thereby play a role in sustaining cachexia. We found that parasites replicate in the same region of the distal jejunum/proximal ileum throughout acute infection, inducing the development of secondary lymphoid structures and severe, regional inflammation. Small intestine pathology was resolved by 5 weeks post-infection. However, changes in the commensal populations, notably an outgrowth of Clostridia spp., were sustained in chronic infection. Importantly, uninfected animals co-housed with infected mice display similar changes in commensal microflora but never display symptoms of cachexia, indicating that altered commensals are not sufficient to explain the cachexia phenotype alone. These studies indicate that Toxoplasma infection is a novel and robust model to study the immune-metabolic interactions that contribute to chronic cachexia development, pathology and potential reversal. [ABSTRACT FROM AUTHOR]

Published

2018

8. Endoluminal ultrasound applicators for MR-guided thermal ablation of pancreatic tumors: Preliminary design and evaluation in a porcine pancreas model.

Author

Adams, Matthew S., Salgaonkar, Vasant A., Plata Camargo, Juan, Jones, Peter D., Pascal Tenorio, Aurea, Chen, Hsin Yu, Bouley, Donna M., Sommer, Graham, Pauly, Kim Butts, and Diederich, Chris J.

Subjects

*PANCREATIC cancer diagnosis, *PANCREATIC cancer treatment, *PANCREAS, *TRANSDUCERS, *HYDRAULICS, *MAGNETIC resonance imaging

Abstract

Purpose: Endoluminal ultrasound may serve as a minimally invasive option for delivering thermal ablation to pancreatic tumors adjacent to the stomach or duodenum. The objective of this study was to explore the basic feasibility of this treatment strategy through the design, characterization, and evaluation of proof-of-concept endoluminal ultrasound applicators capable of placement in the gastrointestinal (GI) lumen for volumetric pancreas ablation under MR guidance. Methods: Two variants of the endoluminal applicator, each containing a distinct array of two independently powered transducers (10 × 10 mm 3.2 MHz planar; or 8 × 10 × 20 mm radius of curvature 3.3 MHz curvilinear geometries) at the distal end of a meter long flexible catheter assembly, were designed and fabricated. Transducers and circulatory water flow for acoustic coupling and luminal cooling were contained by a low-profile polyester balloon covering the transducer assembly fixture. Each applicator incorporated miniature spiral MR coils and mechanical features (guiding tips and hinges) to facilitate tracking and insertion through the GI tract under MRI guidance. Acoustic characterization of each device was performed using radiation force balance and hydrophone measurements. Device delivery into the upper GI tract, adjacent to the pancreas, and heating characteristics for treatment of pancreatic tissue were evaluated in MR-guided ex vivo and in vivo porcine experiments. MR guidance was utilized for anatomical target identification, tracking/positioning of the applicator, and MR temperature imaging (MRTI) for PRF-based multislice thermometry, implemented in the real-time RTHawk software environment. Results: Force balance and hydrophone measurements indicated efficiencies of 48.8% and 47.8% and −3 dB intensity beam-widths of 3.2 and 1.2 mm for the planar and curvilinear transducers, respectively. Ex vivo studies on whole-porcine carcasses revealed capabilities of producing ablative temperature rise (ΔT > 15 °C) contours in pancreatic tissue 4-40 mm long and 4-28 mm wide for the planar transducer applicator (1-13 min sonication duration, ~4 W/cm² applied acoustic intensity). Curvilinear transducers produced more selective heating, with a narrower ΔT > 15 °C contour length and width of up to 1-24 mm and 2-7 mm, respectively (1-7 min sonication duration, ~4 W/cm² applied acoustic intensity). Active tracking of the miniature spiral coils was achieved using a Hadamard encoding tracking sequence, enabling real-time determination of each coil's coordinates and automated prescription of imaging planes for thermometry. In vivo MRTI-guided heating trials in three pigs demonstrated capability of ~20 °C temperature elevation in pancreatic tissue at 2 cm depths from the applicator, with 5-7 W/cm² applied intensity and 6-16 min sonication duration. Dimensions of thermal lesions in the pancreas ranged from 12 to 28 mm, 3 to 10 mm, and 5 to 10 mm in length, width, and depth, respectively, as verified through histological analysis of tissue sections. Multiple-baseline reconstruction and respiratory-gated acquisition were demonstrated to be effective strategies in suppressing motion artifacts for clear evolution of temperature profiles during MRTI in the in vivo studies. Conclusions: This study demonstrates the technical feasibility of generating volumetric ablation in pancreatic tissue using endoluminal ultrasound applicators positioned in the stomach lumen. MR guidance facilitates target identification, device tracking/positioning, and treatment monitoring through real-time multislice PRF-based thermometry. [ABSTRACT FROM AUTHOR]

Published

2016

9. The adherens junctions control susceptibility to Staphylococcus aureus α-toxin.

Author

Popov, Lauren M., Marceau, Caleb D., Starkl, Philipp M., Lumb, Jennifer H., Shah, Jimit, Guerrera, Diego, Cooper, Rachel L., Merakou, Christina, Bouley, Donna M., Wenxiang Meng, Hiroshi Kiyonari, Masatoshi Takeichi, Galli, Stephen J., Bagnoli, Fabio, Citi, Sandra, Carette, Jan E., and Amieva, Manuel R.

Subjects

*STAPHYLOCOCCUS aureus, *MICROCOCCACEAE, *CELL junctions, *ADHERENS junctions, *INFECTION

Abstract

Staphylococcus aureus is both a transient skin colonizer and a formidable human pathogen, ranking among the leading causes of skin and soft tissue infections as well as severe pneumonia. The secreted bacterial α-toxin is essential for S. aureus virulence in these epithelial diseases. To discover host cellular factors required for α-toxin cytotoxicity, we conducted a genetic screen using mutagenized haploid human cells. Our screen identified a cytoplasmic member of the adherens junctions, plekstrin-homology domain containing protein 7 (PLEKHA7), as the second most significantly enriched gene after the known α-toxin receptor, a disintegrin and metalloprotease 10 (ADAM10). Here we report a new, unexpected role for PLEKHA7 and several components of cellular adherens junctions in controlling susceptibility to S. aureus α-toxin.We find that despite being injured by α-toxin pore formation, PLEKHA7 knockout cells recover after intoxication. By infecting PLEKHA7-/- mice with methicillin-resistant S. aureus USA300 LAC strain, we demonstrate that this junctional protein controls disease severity in both skin infection and lethal S. aureus pneumonia. Our results suggest that adherens junctions actively control cellular responses to a potent pore-forming bacterial toxin and identify PLEKHA7 as a potential nonessential host target to reduce S. aureus virulence during epithelial infections. [ABSTRACT FROM AUTHOR]

Published

2015

10. Next-Generation NAMPT Inhibitors Identified by Sequential High-Throughput Phenotypic Chemical and Functional Genomic Screens.

Author

Matheny, Christina?J., Wei, Michael?C., Bassik, Michael?C., Donnelly, Alicia?J., Kampmann, Martin, Iwasaki, Masayuki, Piloto, Obdulio, Solow-Cordero, David?E., Bouley, Donna?M., Rau, Rachel, Brown, Patrick, McManus, Michael?T., Weissman, Jonathan?S., and Cleary, Michael?L.

Subjects

*NICOTINAMIDE, *PHOSPHORIBOSYLTRANSFERASES, *HIGH throughput screening (Drug development), *PHENOTYPES, *FUNCTIONAL genomics, *LEUKEMIA

Abstract

Summary: Phenotypic high-throughput chemical screens allow for discovery of small molecules that modulate complex phenotypes and provide lead compounds for novel therapies; however, identification of the mechanistically relevant targets remains a major experimental challenge. We report the application of sequential unbiased high-throughput chemical and ultracomplex small hairpin RNA (shRNA) screens to identify a distinctive class of inhibitors that target nicotinamide phosphoribosyl transferase (NAMPT), a rate-limiting enzyme in the biosynthesis of nicotinamide adenine dinucleotide, a crucial cofactor in many biochemical processes. The lead compound STF-118804 is a highly specific NAMPT inhibitor, improves survival in an orthotopic xenotransplant model of high-risk acute lymphoblastic leukemia, and targets leukemia stem cells. Tandem high-throughput screening using chemical and ultracomplex shRNA libraries, therefore, provides a rapid chemical genetics approach for seamless progression from small-molecule lead identification to target discovery and validation. [Copyright &y& Elsevier]

Published

2013

11. Loss of Anterior Gradient 2 (Agr2) Expression Results in Hyperplasia and Defective Lineage Maturation in the Murine Stomach.

Author

Gupta, Aparna, Wodziak, Dariusz, Tun, May, Bouley, Donna M., and Lowe, Anson W.

Subjects

*HYPERPLASIA, *TISSUE-specific antibodies, *STEM cells, *CELL lines, *HOMEOSTASIS, *PROGENITOR cells, *PROLIFERATING cell nuclear antigen

Abstract

Recent studies of epithelial tissues have revealed the presence of tissue-specific stem cells that are able to establish multiple cell lineages within an organ. The stem cells give rise to progenitors that replicate before differentiating into specific cell lineages. The mechanism by which homeostasis is established between proliferating stem or progenitor cells and terminally differentiated cells is unclear. This study demonstrates that Agr2 expression by mucous neck cells in the stomach promotes the differentiation of multiple cell lineages while also inhibiting the proliferation of stem or progenitor cells. When Agr2 expression is absent, gastric mucous neck cells increased in number as does the number of proliferating cells. Agr2 expression loss also resulted in the decline of terminally differentiated cells, which was supplanted by cells that exhibited nuclear SOX9 labeling. Sox9 expression has been associated with progenitor and stem cells. Similar effects of the Agr2 null on cell proliferation in the intestine were also observed. Agr2 consequently serves to maintain the balance between proliferating and differentiated epithelial cells. [ABSTRACT FROM AUTHOR]

Published

2013

12. Caspase-11 increases susceptibility to Salmonella infection in the absence of caspase-1.

Author

Broz, Petr, Ruby, Thomas, Belhocine, Kamila, Bouley, Donna M., Kayagaki, Nobuhiko, Dixit, Vishva M., and Monack, Denise M.

Subjects

*CASPASES, *DISEASE susceptibility, *SALMONELLA diseases, *INTERLEUKIN-18, *OLIGOMERIZATION, *TOLL-like receptors

Abstract

Inflammasomes are cytosolic multiprotein complexes assembled by intracellular nucleotide-binding oligomerization domain (NOD)-like receptors (NLRs) and they initiate innate immune responses to invading pathogens and danger signals by activating caspase-1 (ref. 1). Caspase-1 activation leads to the maturation and release of the pro-inflammatory cytokines interleukin (IL)-1? and IL-18, as well as lytic inflammatory cell death known as pyroptosis. Recently, a new non-canonical inflammasome was described that activates caspase-11, a pro-inflammatory caspase required for lipopolysaccharide-induced lethality. This study also highlighted that previously generated caspase-1 knockout mice lack a functional allele of Casp11 (also known as Casp4), making them functionally Casp1?Casp11 double knockouts. Previous studies have shown that these mice are more susceptible to infections with microbial pathogens, including the bacterial pathogen Salmonella enterica serovar Typhimurium (S. typhimurium), but the individual contributions of caspase-1 and caspase-11 to this phenotype are not known. Here we show that non-canonical caspase-11 activation contributes to macrophage death during S. typhimurium infection. Toll-like receptor 4 (TLR4)-dependent and TIR-domain-containing adaptor-inducing interferon-? (TRIF)-dependent interferon-? production is crucial for caspase-11 activation in macrophages, but is only partially required for pro-caspase-11 expression, consistent with the existence of an interferon-inducible activator of caspase-11. Furthermore, Casp1?/? mice were significantly more susceptible to infection with S. typhimurium than mice lacking both pro-inflammatory caspases (Casp1?/??Casp11?/?). This phenotype was accompanied by higher bacterial counts, the formation of extracellular bacterial microcolonies in the infected tissue and a defect in neutrophil-mediated clearance. These results indicate that caspase-11-dependent cell death is detrimental to the host in the absence of caspase-1-mediated innate immunity, resulting in extracellular replication of a facultative intracellular bacterial pathogen. [ABSTRACT FROM AUTHOR]

Published

2012

13. Tumor Galectin-1 Mediates Tumor Growth and Metastasis through Regulation of T-Cell Apoptosis.

Author

Banh, Alice, Jing Zhang, Hongbin Cao, Bouley, Donna M., Kwok, Shirley, Kong, Christina, Giaccia, Amato J., Koong, Albert C., and Quynh-Thu Le

Subjects

*HYPOXEMIA, *NEOVASCULARIZATION, *APOPTOSIS, *PROTEINS, *CANCER

Abstract

Galectin-1 (Gal-1), a carbohydrate-binding protein whose secretion is enhanced by hypoxia, promotes tumor aggressiveness by promoting angiogenesis and T-cell apoptosis. However, the importance of tumor versus host Gal-1 in tumor progression is undefined. Here we offer evidence that implicates tumor Gal-1 and its modulation of T-cell immunity in progression. Comparing Gal-1--deficient mice as hosts for Lewis lung carcinoma cells where Gal-1 levels were preserved or knocked down, we found that tumor Gal-1 was more critical than host Gal-1 in promoting tumor growth and spontaneous metastasis. Enhanced growth and metastasis associated with Gal-1 related to its immunomodulatory function, insofar as the benefits of Gal-1 expression to Lewis lung carcinoma growth were abolished in immunodeficient mice. In contrast, angiogenesis, as assessed by microvessel density count, was similar between tumors with divergent Gal-1 levels when examined at a comparable size. Our findings establish that tumor rather than host Gal-1 is responsible for mediating tumor progression through intratumoral immunomodulation, with broad implications in developing novel targeting strategies for Gal-1 in cancer. Cancer Res; 71(13); 4423-31. ©2011 AACR. [ABSTRACT FROM AUTHOR]

Published

2011

14. 173. Evaluation of thermal and cryo lesions by diffusion-weighted MRI

Author

Chen, Jing, Daniel, Bruce L., Bouley, Donna M., Sommer, Graham, Kaye, Elena A., and Pauly, Kim Butts

Published

2006

15. The RGD Domain of Human Osteopontin Promotes Tumor Growth and Metastasis through Activation of Survival Pathways.

Author

Courter, Donald, Hongbin Cao, Kwok, Shirley, Kong, Christina, Banh, Alice, Peiwen Kuo, Bouley, Donna M., Vice, Carmen, Brustugun, Odd Terje, Denko, Nicholas C., Koong, Albert C., Giaccia, Amato, and Quynh-Thu Le

Subjects

*OSTEOPONTIN, *CELL adhesion molecules, *PHOSPHOPROTEINS, *TUMORS, *CANCER invasiveness, *METASTASIS, *TUMOR growth, *HYPEROXIA, *APOPTOSIS

Abstract

Bacκground: Human osteopontin (OPN), a κnown tumor associated protein, exists in different isoforms, whose function is unclear. It also possesses a RGD domain, which has been implicated in diverse function. Here, we use genetic approaches to systematically investigate the function of the RGD domain in different OPN isoforms on tumor progression and metastasis for 2 different solid tumor models. Methodology/Principal Findings: Using isoform-specific qRT-PCR, we found that OPN-A and B were the main isoforms overexpressed in evaluated human tumors, which included 4 soft tissue sarcomas, 24 lung and 30 head and necκ carcinomas. Overexpression of either OPN-A or B in two different cell types promoted local tumor growth and lung metastasis in SCID mouse xenografts. However, expression of either isoform with the RGD domain either mutated or deleted decreased tumor growth and metastasis, and resulted in increased apoptosis by TUNEL staining. In vitro, whereas mutation of the RGD domain did not affect cell-cell adhesion, soft agar growth or cell migration, it increased apoptosis under hypoxia and serum starvation. This effect could be mitigated when the RGD mutant cells were treated with condition media containing WT OPN. Mechanistically, the RGD region of OPN inhibited apoptosis by inducing NF-κB activation and FAκ phosphorylation. Inhibition of NF-κB (by siRNA to the p65 subunit) or FAκ activation (by a inhibitor) significantly increased apoptosis under hypoxia in WT OPN cells, but not in RGD mutant cells. Conclusion/Significance: Unliκe prior reports, our data suggest that the RGD domain of both OPN-A and B promote tumor growth and metastasis mainly by protecting cells against apoptosis under stressed conditions and not via migration or invasion. Future inhibitors directed against OPN should target multiple isoforms and should inhibit cell survival mechanisms that involve the RGD domain, FAκ phosphorylation and NF-κB activation. [ABSTRACT FROM AUTHOR]

Published

2010

16. Short-term stress enhances cellular immunity and increases early resistance to squamous cell carcinoma

Author

Dhabhar, Firdaus S., Saul, Alison N., Daugherty, Christine, Holmes, Tyson H., Bouley, Donna M., and Oberyszyn, Tatiana M.

Subjects

*PSYCHOLOGICAL stress, *CELLULAR immunity, *SQUAMOUS cell carcinoma, *PHYSIOLOGICAL effects of ultraviolet radiation, *CYTOKINES, *CHEMOKINES, *GENE expression, *IMMUNE response, *FLOW cytometry

Abstract

Abstract: In contrast to chronic/long-term stress that suppresses/dysregulates immune function, an acute/short-term fight-or-flight stress response experienced during immune activation can enhance innate and adaptive immunity. Moderate ultraviolet-B (UV) exposure provides a non-invasive system for studying the naturalistic emergence, progression and regression of squamous cell carcinoma (SCC). Because SCC is an immunoresponsive cancer, we hypothesized that short-term stress experienced before UV exposure would enhance protective immunity and increase resistance to SCC. Control and short-term stress groups were treated identically except that the short-term stress group was restrained (2.5h) before each of nine UV-exposure sessions (minimum erythemal dose, 3-times/week) during weeks 4–6 of the 10-week UV exposure protocol. Tumors were measured weekly, and tissue collected at weeks 7, 20, and 32. Chemokine and cytokine gene expression was quantified by real-time PCR, and CD4+ and CD8+ T cells by flow cytometry and immunohistochemistry. Compared to controls, the short-term stress group showed greater cutaneous T-cell attracting chemokine (CTACK)/CCL27, RANTES, IL-12, and IFN-γ gene expression at weeks 7, 20, and 32, higher skin infiltrating T cell numbers (weeks 7 and 20), lower tumor incidence (weeks 11–20) and fewer tumors (weeks 11–26). These results suggest that activation of short-term stress physiology increased chemokine expression and T cell trafficking and/or function during/following UV exposure, and enhanced Type 1 cytokine-driven cell-mediated immunity that is crucial for resistance to SCC. Therefore, the physiological fight-or-flight stress response and its adjuvant-like immuno-enhancing effects, may provide a novel and important mechanism for enhancing immune system mediated tumor-detection/elimination that merits further investigation. [Copyright &y& Elsevier]

Published

2010

17. The mouse polyubiquitin gene UbC is essential for fetal liver development, cell-cycle progression and stress tolerance.

Author

Kwon-Yul Ryu, Maehr, René, Gilchrist, Catherine A., Long, Michael A., Bouley, Donna M., Mueller, Britta, Ploegh, Hidde L., and Kopito, Ron R.

Subjects

*GENES, *MAMMALS, *UBIQUITIN, *PROTEINS, *CELL proliferation, *APOPTOSIS

Abstract

UbC is one of two stress-inducible polyubiquitin genes in mammals and is thought to supplement the constitutive UbA genes in maintaining cellular ubiquitin (Ub) levels during episodes of cellular stress. We have generated mice harboring a targeted disruption of the UbC gene. UbC−/− embryos die between embryonic days 12.5 and 14.5 in utero, most likely owing to a severe defect in liver cell proliferation. Mouse embryonic fibroblasts from UbC−/− embryos exhibit reduced growth rates, premature senescence, increased apoptosis and delayed cell-cycle progression, with slightly, but significantly, decreased steady-state Ub levels. UbC−/− fibroblasts are hypersensitive to proteasome inhibitors and heat shock, and unable to adequately increase Ub levels in response to these cellular stresses. Most, but not all of the UbC−/− phenotypes can be rescued by providing additional Ub from a poly hemagglutinin-tagged Ub minigene expressed from the Hprt locus. We propose that UbC is regulated by a process that senses Ub pool dynamics. These data establish that UbC constitutes an essential source of Ub during cell proliferation and stress that cannot be compensated by other Ub genes. [ABSTRACT FROM AUTHOR]

Published

2007

18. RabGEF1 is a negative regulator of mast cell activation and skin inflammation.

Author

See-Ying Tam, Tsai, Mindy, Snouwaert, John N., Kalesnikoff, Janet, Scherrer, Didier, Nakae, Susumu, Chatterjea, Devavani, Bouley, Donna M., and Galli, Stephen J.

Subjects

*IMMUNOLOGY, *PROTEINS, *MAST cells, *SKIN inflammation, *PROTEIN kinases

Abstract

Mast cell activation induced by aggregation of FceRI receptors with immunoglobulin E and antigen is mediated through the activation of multiple protein kinase cascades. Here we report that the regulatory protein RabGEF1 bound to Ras and negatively regulated Ras activation and its 'downstream' effector pathways in FceRI-dependent mast cell activation. RabGEF1-deficient mast cells showed enhanced degranulation and release of lipid mediators and cytokines in response to FceRI aggregation. RabGEF1-deficient mice developed severe skin inflammation and had increased numbers of mast cells. Thus, RabGEF1 is a negative regulator of FceRI-dependent mast cell activation, and a lack of RabGEF1 results in the development of skin inflammation in vivo. [ABSTRACT FROM AUTHOR]

Published

2004

19. The Mouse Polyubiquitin Gene Ubb Is Essential for Meiotic Progression.

Author

Kwon-Yul Ryu, Sinnar, Shamim A., Reinholdt, Laura G., Vaccari, Sergio, Hall, Susan, Garcia, Manuel A., Zaitseva, Tatiana S., Bouley, Donna M., Boekelheide, Kim, Handel, Mary Ann, Conti, Marco, and Kopito, Ron R.

Subjects

*UBIQUITIN, *GENES, *GERM cells, *MEIOSIS, *HYPOGONADISM, *SCHIZOSACCHAROMYCES pombe, *EUKARYOTIC cells, *LABORATORY mice

Abstract

Ubiquitin is encoded in mice by two polyubiquitin genes, Ubb and Ubc, that are considered to be stress inducible and two constitutively expressed monoubiquitin (Uba) genes. Here we report that targeted disruption of Ubb results in male and female infertility due to failure of germ cells to progress through meiosis I and hypogonadism. In the absence of Ubb, spermatocytes and oocytes arrest during meiotic prophase, before metaphase of the first meiotic division. Although cellular ubiquitin levels are believed to be maintained by a combination of functional redundancy among the four ubiquitin genes, stress inducibility of the two polyubiquitin genes, and ubiquitin recycling by proteasome- associated isopeptidases, our results indicate that ubiquitin is required for and consumed during meiotic progression. The striking similarity of the meiotic phenotype in Ubb-/- germ cells to the sporulation defect in fission yeast (Schizosaccharomyces pombe) lacking a polyubiquitin gene suggests that a meiotic role of the polyubiquitin gene has been conserved throughout eukaryotic evolution. [ABSTRACT FROM AUTHOR]

Published

2008