Your search keyword '"Phillips, Bryan"' showing total 19 results

1. The benefits of local depletion: The centrosome as a scaffold for ubiquitin-proteasome-mediated degradation.

Author

Vora, Setu M. and Phillips, Bryan T.

Published

2016

2. Centrosome-Associated Degradation Limits β-Catenin Inheritance by Daughter Cells after Asymmetric Division.

Author

Vora, Setu and Phillips, Bryan T.

Subjects

*CENTROSOMES, *CATENINS, *CELL division, *CAENORHABDITIS elegans, *CELL determination, *GENETIC transcription

Abstract

Summary Caenorhabditis elegans embryos rapidly diversify cell fate using a modified Wnt/β-catenin signaling strategy to carry out serial asymmetric cell divisions (ACDs). Wnt-dependent ACDs rely on nuclear asymmetry of the transcriptional coactivator SYS-1/β-catenin between daughter cells to differentially activate Wnt-responsive target genes. Here, we investigate how dynamic localization of SYS-1 to mitotic centrosomes influences SYS-1 inheritance in daughter cells and cell-fate outcomes after ACD. Through yeast two-hybrid screening, we identify the centrosomal protein RSA-2 as a SYS-1 binding partner and show that localization of SYS-1 to mitotic centrosomes is dependent on RSA-2. Uncoupling SYS-1 from the centrosome by RSA-2 depletion increases SYS-1 inheritance after ACD and promotes Wnt-dependent cell fate. Photobleaching experiments reveal that centrosome-bound SYS-1 turns over rapidly. Interestingly, disruption of the proteasome leads to an increased accumulation of SYS-1 at the centrosome but disrupts its dynamic turnover. We conclude that centrosomal targeting of SYS-1 promotes its degradation during asymmetric cell division. We propose a model whereby centrosome-associated SYS-1 degradation couples negative regulation with cell-division timing to facilitate SYS-1 clearance from the mother cell at the time of asymmetric division. Based on our observations of centrosomal SYS-1 dynamics, we discuss the possibility that the centrosome may coordinate various cell-cycle-dependent processes by synchronizing mitosis and protein regulation. [ABSTRACT FROM AUTHOR]

Published

2015

3. The tumor suppressor APC differentially regulates multiple β-catenins through the function of axin and CKIα during C. elegans asymmetric stem cell divisions.

Author

Baldwin, Austin T. and Phillips*, Bryan T.

Subjects

*TUMOR suppressor genes, *CATENINS, *AXIN, *STEM cell culture, *CELL division, *CAENORHABDITIS elegans

Abstract

The APC tumor suppressor regulates diverse stem cell processes including gene regulation through Wnt-β-catenin signaling and chromosome stability through microtubule interactions, but how the disparate functions of APC are controlled is not well understood. Acting as part of a Wnt-β-catenin pathway that controls asymmetric cell division, Caenorhabditis elegans APC, APR-1, promotes asymmetric nuclear export of the β-catenin WRM-1 by asymmetrically stabilizing microtubules. Wnt function also depends on a second β-catenin, SYS-1, which binds to the C. elegans TCF POP-1 to activate gene expression. Here, we show that APR-1 regulates SYS-1 levels in asymmetric stem cell division, in addition to its known role in lowering nuclear levels of WRM-1. We demonstrate that SYS-1 is also negatively regulated by the C. elegans homolog of casein kinase 1a (CKIa), KIN-19. We show that KIN-19 restricts APR-1 localization, thereby regulating nuclear WRM-1. Finally, the polarity of APR-1 cortical localization is controlled by PRY-1 (C. elegans Axin), such that PRY-1 controls the polarity of both SYS-1 and WRM-1 asymmetries. We propose a model whereby Wnt signaling, through CKIa, regulates the function of two distinct pools of APC -- one APC pool negatively regulates SYS-1, whereas the second pool stabilizes microtubules and promotes WRM-1 nuclear export. [ABSTRACT FROM AUTHOR]

Published

2014

4. A New Look at TCF and β-Catenin through the Lens of a Divergent C. elegans Wnt Pathway

Author

Phillips, Bryan T. and Kimble, Judith

Subjects

*CELLULAR signal transduction, *CELL adhesion molecules, *CAENORHABDITIS elegans, *SYMMETRY (Biology), *BIOLOGICAL divergence, *CYTOLOGY

Abstract

The canonical Wnt/β-catenin pathway is extensively characterized, broadly conserved, and clinically important. In this review, we describe the C. elegans Wnt/β-catenin asymmetry pathway and suggest that some of its unusual features may have important implications for the canonical Wnt/β-catenin pathway. [Copyright &y& Elsevier]

Published

2009

5. The C. elegans SYS-1 Protein Is a Bona Fide β-Catenin

Author

Liu, Jing, Phillips, Bryan T., Amaya, Maria F., Kimble, Judith, and Xu, Wenqing

Subjects

*CARRIER proteins, *CAENORHABDITIS elegans, *PROTEINS, *CRYSTALS, *POLYPEPTIDES

Abstract

Summary: C. elegans SYS-1 has key functional characteristics of a canonical β-catenin, but no significant sequence similarity. Here, we report the SYS-1 crystal structure, both on its own and in a complex with POP-1, the C. elegans TCF homolog. The two structures possess signature features of canonical β-catenin and the β-catenin/TCF complex that could not be predicted by sequence. Most importantly, SYS-1 bears 12 armadillo repeats and the SYS-1/POP-1 interface is anchored by a conserved salt-bridge, the “charged button.” We also modeled structures for three other C. elegans β-catenins to predict the molecular basis of their distinct binding properties. Finally, we generated a phylogenetic tree, using the region of highest structural similarity between SYS-1 and β-catenin, and found that SYS-1 clusters robustly within the β-catenin clade. We conclude that the SYS-1 protein belongs to the β-catenin family and suggest that additional divergent β-catenins await discovery. [Copyright &y& Elsevier]

Published

2008

6. Reciprocal asymmetry of SYS-1/β-catenin and POP-1 ITCF controls asymmetric divisions in Caenorhabditis elegans.

Author

Phillips, Bryan T., Kidd III, Ambrose R., King, Ryan, Hardin, Jeff, and Kimble, Judith

Subjects

*CAENORHABDITIS elegans, *CARRIER proteins, *DNA, *TISSUES, *GENE expression, *CELL division

Abstract

β-Catenins are conserved regulators of metazoan development that function with TCF DNA-binding proteins to activate transcription. In Caenorhabditis elegans, SYS-1β-catenin and POP-1/TCF regulate several asymmetric divisions, including that of the somatic gonadal precursor cell (SGP). In the distal but not the proximal SGP daughter, SYS-1/β-catenin and POP-1/TCF transcriptionally activate ceh-22 to specify the distal fate. Here, we investigate the distribution of SYS-1/β-catenin and its regulation. Using a rescuing transgene, VNS::SYS-1, which fuses VENUS fluorescent protein to SYS-1, we find more VNS::SYS-1 in distal than proximal SGP daughters, a phenomenon we call "SYS-1 asymmetry." In addition, SYS-1 asymmetry is seen in many other tissues, consistent with the idea that SYS-1 regulates asymmetric divisions broadly during C. elegans development. In particular, SYS-1 is more abundant in E than MS. and SYS-1 is critical for the endodermal fate. In all cases, SYS-1 is reciprocal to POP-1 asymmetry: cells with higher SYS-1 have lower POP-1, and vice versa. SYS-1 asymmetry is controlled posttranslationally and relies on frizzled and dishevelled homologs, which also control POP-1 asymmetry. Therefore, upstream regulators modulate the SYS-1 to POP-1 ratio by increasing SYS-1 and decreasing POP-1 within the same cell. By contrast. SYS-1 asymmetry does not rely on WRM-1, which appears specialized for POP-1 asymmetry. We suggest a two-pronged pathway for control of SYS-1:POP-1, which can robustly accomplish differential gene expression in daughters of an asymmetric cell division. [ABSTRACT FROM AUTHOR]

Published

2007

7. Zebrafish msxB, msxC and msxE function together to refine the neural–nonneural border and regulate cranial placodes and neural crest development

Author

Phillips, Bryan T., Kwon, Hye-Joo, Melton, Colt, Houghtaling, Paul, Fritz, Andreas, and Riley, Bruce B.

Subjects

*ZEBRA danio, *CELL growth, *NERVOUS system, *HEREDITY

Abstract

Abstract: The zebrafish muscle segment homeobox genes msxB, msxC and msxE are expressed in partially overlapping domains in the neural crest and preplacodal ectoderm. We examined the roles of these msx genes in early development. Disrupting individual msx genes causes modest variable defects, whereas disrupting all three produces a reproducible severe phenotype, suggesting functional redundancy. Neural crest differentiation is blocked at an early stage. Preplacodal development begins normally, but placodes arising from the msx expression domain later show elevated apoptosis and are reduced in size. Cell proliferation is normal in these tissues. Unexpectedly, Msx-deficient embryos become ventralized by late gastrulation whereas misexpression of msxB dorsalizes the embryo. These effects appear to involve Distal-less (Dlx) protein activity, as loss of dlx3b and dlx4b suppresses ventralization in Msx-depleted embryos. At the same time, Msx-depletion restores normal preplacodal gene expression to dlx3b-dlx4b mutants. These data suggest that mutual antagonism between Msx and Dlx proteins achieves a balance of function required for normal preplacodal differentiation and placement of the neural–nonneural border. [Copyright &y& Elsevier]

Published

2006

8. Changes in the Fish Assemblage of Bear Creek (Tennessee River Drainage) Alabama and Mississippi: 1968--2000.

Author

Phillips, Bryan W. and Johnston, Carol E.

Subjects

*FISH surveys, *FISHES, *SPECIES

Abstract

Since a comprehensive fish survey in 1968, four impoundments have been constructed in the Bear Creek (Tennessee River drainage) watershed in Alabama (Wall 1968). Data from this original study were compared to a recent survey in order to determine if any changes in fish species composition had occurred during the approximately 30 year time period. A comparison of similarity for 44 collections showed low similarity between the two surveys for a large percentage of sites visited (86% for Jaccard's Similarity and 62% for Morisita Similarity). Sites with low similarity between survey dates were typically associated with impoundments. Most species missing in the recent survey include species considered sensitive, such as cyprinids and percids. Species that have increased since 1968 include centrarchids, a group typically tolerant of impoundment and environmental change. Virtually all fish species composition differences indicate a less pristine fish assemblage in the more contemporary survey, suggesting that recent factors have had a negative effect on the fish assemblage of Bear Creek. [ABSTRACT FROM AUTHOR]

Published

2004

9. A direct role for Fgf but not Wnt in otic placode induction.

Author

Phillips, Bryan T., Storch, Elly M., Lekven, Arne C., and Riley, Bruce B.

Subjects

*PLACODES, *TISSUES, *VERTEBRATES, *FIBROBLAST growth factors, *ZEBRA danio, *CELLS

Abstract

Induction of the otic placode, which gives rise to all tissues comprising the inner ear, is a fundamental aspect of vertebrate development. A number of studies indicate that fibroblast growth factor (Fgf), especially Fgf3, is necessary and sufficient for otic induction. However, an alternative model proposes that Fgf must cooperate with Wnt8 to induce otic differentiation. Using a genetic approach in zebrafish, we tested the roles of Fgf3, Fgf8 and Wnt8. We demonstrate that localized misexpression of either Fgf3 or Fgf8 is sufficient to induce ectopic otic placodes and vesicles, even in embryos lacking Wnt8. Wnt8 is expressed in the hindbrain around the time of otic induction, but loss of Wnt8 merely delays expression of preotic markers and otic vesicles form eventually. The delay in otic induction correlates closely with delayed expression of fgf3 and fgf8 in the hindbrain. Localized misexpression of Wnt8 is insufficient to induce ectopic otic tissue. By contrast, global misexpression of Wnt8 causes development of supernumerary placodes/vesicles, but this reflects posteriorization of the neural plate and consequent expansion of the hindbrain expression domains of Fgf3 and Fgf8. Embryos that misexpress Wnt8 globally but are depleted for Fgf3 and Fgf8 produce no otic tissue. Finally, cells in the preotic ectoderm express Fgf (but not Wnt) reporter genes. Thus, preotic cells respond directly to Fgf but not Wnt8. We propose that Wnt8 serves to regulate timely expression of Fgf3 and Fgf8 in the hindbrain, and that Fgf from the hindbrain then acts directly on preplacodal cells to induce otic differentiation. [ABSTRACT FROM AUTHOR]

Published

2004

10. Ringing in the new ear: resolution of cell interactions in otic development

Author

Riley, Bruce B. and Phillips, Bryan T.

Subjects

*INNER ear, *EMBRYOLOGISTS, *STEM cells, *NEUROBIOLOGY

Abstract

The vertebrate inner ear is a marvel of structural and functional complexity, which is all the more remarkable because it develops from such a simple structure, the otic placode. Analysis of inner ear development has long been a fascination of experimental embryologists, who sought to understand cellular mechanisms of otic placode induction. More recently, however, molecular and genetic approaches have made the inner ear a useful model system for studying a much broader range of basic developmental mechanisms, including cell fate specification and differentiation, axial patterning, epithelial morphogenesis, cytoskeletal dynamics, stem cell biology, neurobiology, physiology, etc. Of course, there has also been tremendous progress in understanding the functions and processes peculiar to the inner ear. The goal of this review is to recount how historical approaches have shaped our understanding of the signaling interactions controlling early otic development; to discuss how new findings have led to fundamental new insights; and to point out new problems that need to be resolved in future research. [Copyright &y& Elsevier]

Published

2003

11. Assessing the impact of community-based interventions on hypertension and diabetes management in three Minnesota communities: Findings from the prospective evaluation of US HealthRise programs.

Author

Fullman, Nancy, Cowling, Krycia, Flor, Luisa S., Wilson, Shelley, Bhatt, Paurvi, Bryant, Miranda F., Camarda, Joseph N., Colombara, Danny V., Daly, Jessica, Gabert, Rose K., Harris, Katie Panhorst, Johanns, Casey K., Mandile, Charlie, Marshall, Susan, McNellan, Claire R., Mulakaluri, Vasudha, Phillips, Bryan K., Reitsma, Marissa B., Sadighi, Naomi, and Tamene, Tsega

Subjects

*COMMUNITIES, *SYSTOLIC blood pressure, *COMMUNITY health workers, *SUSTAINABILITY, *HYPERTENSION, *DIABETES

Abstract

Background: Community-based health interventions are increasingly viewed as models of care that can bridge healthcare gaps experienced by underserved communities in the United States (US). With this study, we sought to assess the impact of such interventions, as implemented through the US HealthRise program, on hypertension and diabetes among underserved communities in Hennepin, Ramsey, and Rice Counties, Minnesota. Methods and findings: HealthRise patient data from June 2016 to October 2018 were assessed relative to comparison patients in a difference-in-difference analysis, quantifying program impact on reducing systolic blood pressure (SBP) and hemoglobin A1c, as well as meeting clinical targets (< 140 mmHg for hypertension, < 8% Al1c for diabetes), beyond routine care. For hypertension, HealthRise participation was associated with SBP reductions in Rice (6.9 mmHg [95% confidence interval: 0.9–12.9]) and higher clinical target achievement in Hennepin (27.3 percentage-points [9.8–44.9]) and Rice (17.1 percentage-points [0.9 to 33.3]). For diabetes, HealthRise was associated with A1c decreases in Ramsey (1.3 [0.4–2.2]). Qualitative data showed the value of home visits alongside clinic-based services; however, challenges remained, including community health worker retention and program sustainability. Conclusions: HealthRise participation had positive effects on improving hypertension and diabetes outcomes at some sites. While community-based health programs can help bridge healthcare gaps, they alone cannot fully address structural inequalities experienced by many underserved communities. [ABSTRACT FROM AUTHOR]

Published

2023

12. Unique and redundant β-catenin regulatory roles of two Dishevelled paralogs during C. elegans asymmetric cell division.

Author

Baldwin, Austin T., Clemons, Amy M., and Phillips, Bryan T.

Subjects

*WNT signal transduction, *CELLULAR signal transduction, *WNT proteins, *CAENORHABDITIS elegans, *PHYSIOLOGICAL effects of proteins

Abstract

The Wnt/β-catenin signaling pathway is utilized across metazoans. However, the mechanism of signal transduction, especially dissociation of the β-catenin destruction complex by Dishevelled proteins, remains controversial. Here, we describe the function of the Dishevelled paralogs DSH-2 and MIG-5 in the Wnt/β-catenin asymmetry (WβA) pathway in Caenorhabditis elegans, where WβA drives asymmetric cell divisions throughout development. We find that DSH-2 and MIG-5 redundantly regulate cell fate in hypodermal seam cells. Similarly, both DSH-2 and MIG-5 are required for positive regulation of SYS-1 (a C. elegans β-catenin), but MIG-5 has a stronger effect on the polarity of SYS-1 localization. We show that MIG-5 controls cortical APR-1 (the C. elegans APC) localization. DSH-2 and MIG-5 both regulate the localization of WRM-1 (another C. elegans β-catenin), acting together as negative regulators of WRM-1 nuclear localization. Finally, we demonstrate that overexpression of DSH-2 or MIG-5 in seam cells leads to stabilization of SYS-1 in the anterior seam daughter, solidifying the Dishevelled proteins as positive regulators of SYS-1. Overall, we have further defined the role of Dishevelled in the WβA signaling pathway, and demonstrated that DSH-2 and MIG-5 regulate cell fate, β-catenin nuclear levels and the polarity of β-catenin regulation. [ABSTRACT FROM AUTHOR]

Published

2016

13. Identifying gaps in the continuum of care for cardiovascular disease and diabetes in two communities in South Africa: Baseline findings from the HealthRise project.

Author

Wollum, Alexandra, Gabert, Rose, McNellan, Claire R., Daly, Jessica M., Reddy, Priscilla, Bhatt, Paurvi, Bryant, Miranda, Colombara, Danny V., Naidoo, Pamela, Ngongo, Belinda, Nyembezi, Anam, Petersen, Zaino, Phillips, Bryan, Wilson, Shelley, Gakidou, Emmanuela, and Duber, Herbert C.

Subjects

*CARDIOVASCULAR disease treatment, *HEALTH facilities, *TREATMENT of diabetes, *NON-communicable diseases, *HYPERCHOLESTEREMIA, *HEALTH outcome assessment

Abstract

Background: The HealthRise initiative seeks to implement and evaluate innovative community-based strategies for diabetes, hypertension and hypercholesterolemia along the entire continuum of care (CoC)-from awareness and diagnosis, through treatment and control. In this study, we present baseline findings from HealthRise South Africa, identifying gaps in the CoC, as well as key barriers to care for non-communicable diseases (NCDs). Methods: This mixed-methods needs assessment utilized national household data, health facility surveys, focus group discussions, and key informant interviews in Umgungundlovu and Pixley ka Seme districts. Risk factor and disease prevalence were estimated from the South Africa National Health and Nutrition Examination Survey. Health facility surveys were conducted at 86 facilities, focusing on essential intervention, medications and standard treatment guidelines. Quantitative results are presented descriptively, and qualitative data was analyzed using a framework approach. Results: 46.8% of the population in Umgungundlovu and 51.0% in Pixley ka Seme were hypertensive. Diabetes was present in 11.0% and 9.7% of the population in Umgungundlovu and Pixley ka Seme. Hypercholesterolemia was more common in Pixley ka Seme (17.3% vs. 11.1%). Women and those of Indian descent were more likely to have diabetes. More than half of the population was found to be overweight, and binge drinking, inactivity and smoking were all common. More than half of patients with hypertension were unaware of their disease status (51.6% in Pixley ka Seme and 51.3% in Umgungundlovu), while the largest gap in the diabetes CoC occurred between initiation of treatment and achieving disease control. Demand-side barriers included lack of transportation, concerns about confidentiality, perceived discrimination and long wait times. Supply-side barriers included limited availability of testing equipment, inadequate staffing, and pharmaceutical stock outs. Conclusion: In this baseline assessment of two South African health districts we found high rates of undiagnosed hypercholesterolemia and hypertension, and poor control of hypercholesterolemia, hypertension, and diabetes. The HealthRise Initiative will need to address key supply- and demand-side barriers in an effort to improve important NCD outcomes. [ABSTRACT FROM AUTHOR]

Published

2018

14. Identifying gaps in the continuum of care for hypertension and diabetes in two Indian communities.

Author

Gabert, Rose, Ng, Marie, Sogarwal, Ruchi, Bryant, Miranda, Deepu, R. V., McNellan, Claire R., Mehra, Sunil, Phillips, Bryan, Reitsma, Marissa, Thomson, Blake, Wilson, Shelley, Wollum, Alexandra, Gakidou, Emmanuela, and Duber, Herbert C.

Subjects

*HYPERTENSION, *CARDIOVASCULAR disease diagnosis, *DIAGNOSIS of diabetes, *BLOOD sugar monitors, *DIASTOLE (Cardiac cycle), *HEALTH outcome assessment, *ASIANS, *COMPARATIVE studies, *CONTINUUM of care, *DIABETES, *FOCUS groups, *INTERVIEWING, *RESEARCH methodology, *MEDICAL cooperation, *QUALITY assurance, *RESEARCH, *SURVEYS, *QUALITATIVE research, *EVALUATION research

Abstract

Background: Non-communicable diseases (NCDs) represent the largest, and fastest growing, burden of disease in India. This study aimed to quantify levels of diagnosis, treatment, and control among hypertensive and diabetic patients, and to describe demand- and supply-side barriers to hypertension and diabetes diagnosis and care in two Indian districts, Shimla and Udaipur.Methods: We conducted household and health facility surveys, as well as qualitative focus group discussions and interviews. The household survey randomly sampled individuals aged 15 and above in rural and urban areas in both districts. The survey included questions on NCD knowledge, history, and risk factors. Blood pressure, weight, height, and blood glucose measurements were obtained. The health facility survey was administered in 48 health care facilities, focusing on NCD diagnosis and treatment capacity, including staffing, equipment, and pharmaceuticals. Qualitative data was collected through semi-structured key informant interviews with health professionals and public health officials, as well as focus groups with patients and community members.Results: Among 7181 individuals, 32% either reported a history of hypertension or were found to have a systolic blood pressure ≥ 140 mmHg and/or diastolic ≥90 mmHg. Only 26% of those found to have elevated blood pressure reported a prior diagnosis, and just 42% of individuals with a prior diagnosis of hypertension were found to be normotensive. A history of diabetes or an elevated blood sugar (Random blood glucose (RBG) ≥200 mg/dl or fasting blood glucose (FBG) ≥126 mg/dl) was noted in 7% of the population. Among those with an elevated RBG/FBG, 59% had previously received a diagnosis of diabetes. Only 60% of diabetics on treatment were measured with a RBG <200 mg/dl. Lower-level health facilities were noted to have limited capacity to measure blood glucose as well as significant gaps in the availability of first-line pharmaceuticals for both hypertension and diabetes.Conclusions: We found high rates of uncontrolled diabetes and undiagnosed and uncontrolled hypertension. Lower level health facilities were constrained by capacity to test, monitor and treat diabetes and hypertension. Interventions aimed at improving patient outcomes will need to focus on the expanding access to quality care in order to accommodate the growing demand for NCD services. [ABSTRACT FROM AUTHOR]

Published

2017

15. Asymmetric Wnt Pathway Signaling Facilitates Stem Cell-Like Divisions via the Nonreceptor Tyrosine Kinase FRK-1 in Caenorhabditis elegans.

Author

Mila, Danielle, Calderon, Adriana, Baldwin, Austin T., Moore, Kelsey M., Watson, McLane, Phillips, Bryan T., and Putzke, Aaron P.

Subjects

*CELL division, *CELL differentiation, *CELL migration, *PROTEIN-tyrosine kinases, *FATE mapping (Genetics)

Abstract

Asymmetric cell division is critical during development, as it influences processes such as cell fate specification and cell migration. We have characterized FRK-1, a homolog of the mammalian Fer nonreceptor tyrosine kinase, and found it to be required for differentiation and maintenance of epithelial cell types, including the stem cell-like seam cells of the hypodermis. A genomic knockout of frk-1, allele ok760, results in severely uncoordinated larvae that arrest at the L1 stage and have an excess number of lateral hypodermal cells that appear to have lost asymmetry in the stem cell-like divisions of the seam cell lineage. frk-1(ok760) mutants show that there are excess lateral hypodermal cells that are abnormally shaped and smaller in size compared to wild type, a defect that could be rescued only in a manner dependent on the kinase activity of FRK-1. Additionally, we observed a significant change in the expression of heterochronic regulators in frk-1(ok760) mutants. However, frk-1(ok760) mutants do not express late, nonseam hypodermal GFP markers, suggesting the seam cells do not precociously differentiate as adult-hyp7 cells. Finally, our data also demonstrate a clear role for FRK-1 in seam cell proliferation, as eliminating FRK-1 during the L3-L4 transition results in supernumerary seam cell nuclei that are dependent on asymmetric Wnt signaling. Specifically, we observe aberrant POP-1 and WRM-1 localization that is dependent on the presence of FRK-1 and APR-1. Overall, our data suggest a requirement for FRK-1 in maintaining the identity and proliferation of seam cells primarily through an interaction with the asymmetric Wnt pathway. [ABSTRACT FROM AUTHOR]

Published

2015

16. Global, regional, and national levels of neonatal, infant, and under-5 mortality during 1990-2013: a systematic analysis for the Global Burden of Disease Study 2013.

Author

Haidong Wang, Liddell, Chelsea A., Coates, Matthew M., Mooney, Meghan D., Levitz, Carly E., Schumacher, Austin E., Apfel, Henry, lannarone, Marissa, Phillips, Bryan, Lofgren, Katherine T., Sandar, Logan, Dorrington, Rob E., Rakovac, Ivo, Jacobs, Troy A., Xiaofeng Liang, Maigeng Zhou, Jun Zhu, Gonghuan Yang, Yanping Wang, and Shiwei Liu

Subjects

*CHILD mortality, *INFANT mortality, *NEONATAL mortality, *CHILDBIRTH

Abstract

The article discusses a study which examined global trends in neonatal, infant and under-5 mortality from 1990 to 2013. Topics discussed include a reduction in child mortality rate, an increase in the number of child births in 2013 as compared to 1990, and developing countries expected to achieve the Millennium Development Goal 4 (MDG 4).

Published

2014

17. C. elegans HLH-2/E/Daughterless controls key regulatory cells during gonadogenesis

Author

Chesney, Michael A., Lam, Ngan, Morgan, Dyan E., Phillips, Bryan T., and Kimble, Judith

Subjects

*CAENORHABDITIS elegans, *MORPHOGENESIS -- Molecular aspects, *EMBRYONIC stem cells, *CELL lines, *MOLECULAR biology, *GENE expression, *CELL proliferation

Abstract

Abstract: The Caenorhabditis elegans distal tip cell (DTC) provides a niche for germline stem cells in both hermaphrodites and males. The hermaphrodite distal tip cell (hDTC) also provides “leader” function to control gonadal elongation and shape, while in males, leader function is allocated to the linker cell (LC). Therefore, the male distal tip cell (mDTC) serves as a niche but not as a leader. The C. elegans homolog of E/Daughterless, HLH-2, was previously implicated in hDTC specification. Here we report that HLH-2 is also critical for hDTC maintenance, hDTC niche function and hDTC expression of a lag-2/DSL ligand reporter. We also find that HLH-2 functions in males to direct linker cell specification and to promote both mDTC maintenance and the mDTC niche function. We conclude that HLH-2 functions in both sexes to promote leader cell specification and DTC niche function. [Copyright &y& Elsevier]

Published

2009

18. Protein Aggregation and Disaggregation in Cells and Development.

Author

Fassler, Jan S., Skuodas, Sydney, Weeks, Daniel L., and Phillips, Bryan T.

Subjects

*ANIMAL development, *POST-translational modification, *BIOLOGICAL systems, *PROTEINS, *CELL differentiation, *CELL aggregation

Abstract

[Display omitted] • Regulated aggregation affects protein storage, activity and spatial distribution. • Many "bodies" historically connected to cell and development are protein condensates. • Physiological aggregates are regulated, reversible, and often multifunctional. • Chaperones, protein modification, local milieu and co-aggregates alter aggregation. • Exploring multiple experimental systems helps identify regulators of aggregation. Protein aggregation is a feature of numerous neurodegenerative diseases. However, regulated, often reversible, formation of protein aggregates, also known as condensates, helps control a wide range of cellular activities including stress response, gene expression, memory, cell development and differentiation. This review presents examples of aggregates found in biological systems, how they are used, and cellular strategies that control aggregation and disaggregation. We include features of the aggregating proteins themselves, environmental factors, co-aggregates, post-translational modifications and well-known aggregation-directed activities that influence their formation, material state, stability and dissolution. We highlight the emerging roles of biomolecular condensates in early animal development, and disaggregation processing proteins that have recently been shown to play key roles in gametogenesis and embryogenesis. [ABSTRACT FROM AUTHOR]

Published

2021

19. Effect of Different Doses of Caffeine on Anaerobic Performance in Young Boys.

Author

Turley, Kenneth R., Eusse, Paola, Thomas, Myles, Townsend, Jeremy R., Morton, Aaron B., Phillips, Bryan L., and Cullum, Mark G.

Published

2011