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1. Exploring maternal and developmental toxicity of perfluoroalkyl ether acids PFO4DA and PFO5DoA using hepatic transcriptomics and serum metabolomics.

2. Long-chain perfluoroalkylether carboxylic acids PFO5DoA and PFO4DA alter glucose, bile acid, and thyroid hormone homeostasis in fetal rats from 5-day maternal oral exposure.

3. Preventive Human Genome Editing and Enhancement: Candidate Criteria for Governance.

4. Challenging the Boundaries Between Treatment, Prevention, and Enhancement in Human Genome Editing.

5. Using targeted fetal rat testis genomic and endocrine alterations to predict the effects of a phthalate mixture on the male reproductive tract.

6. Public participation in human genome editing research governance: what do scientists think?

7. The public-private research ecosystem in the genome editing era.

8. Maternal and Neonatal Effects of Maternal Oral Exposure to Perfluoro-2-methoxyacetic Acid (PFMOAA) during Pregnancy and Early Lactation in the Sprague-Dawley Rat.

9. Dose Addition Models Accurately Predict the Subacute Effects of a Mixture of Perfluorooctane Sulfonate and Perfluorooctanoic Acid on Japanese Quail (Coturnix japonica) Chick Mortality.

10. Dynamic regulation of pancreatic β cell function and gene expression by the SND1 coregulator in vitro .

11. Dose additive maternal and offspring effects of oral maternal exposure to a mixture of three PFAS (HFPO-DA, NBP2, PFOS) during pregnancy in the Sprague-Dawley rat.

12. The Promise and Reality of Public Engagement in the Governance of Human Genome Editing Research.

13. Cumulative maternal and neonatal effects of combined exposure to a mixture of perfluorooctanoic acid (PFOA) and perfluorooctane sulfonic acid (PFOS) during pregnancy in the Sprague-Dawley rat.

14. Scientists' Views on Scientific Self-Governance for Human Genome Editing Research.

15. In vitro activity of a panel of per- and polyfluoroalkyl substances (PFAS), fatty acids, and pharmaceuticals in peroxisome proliferator-activated receptor (PPAR) alpha, PPAR gamma, and estrogen receptor assays.

16. In Utero Exposure to a Mixture of the Perfluoroalkyl-Isopropyl Pesticide Pyrifluquinazon With Dibutyl Phthalate Cumulatively Disrupts Male Rat Reproductive Development via Different Mechanisms of Action.

17. Developmental toxicity of Nafion byproduct 2 (NBP2) in the Sprague-Dawley rat with comparisons to hexafluoropropylene oxide-dimer acid (HFPO-DA or GenX) and perfluorooctane sulfonate (PFOS).

18. Intestinal Gpr17 deficiency improves glucose metabolism by promoting GLP-1 secretion.

19. A high-fat diet catalyzes progression to hyperglycemia in mice with selective impairment of insulin action in Glut4-expressing tissues.

20. A mixture of 15 phthalates and pesticides below individual chemical no observed adverse effect levels (NOAELs) produces reproductive tract malformations in the male rat.

21. Pilot-scale expanded assessment of inorganic and organic tapwater exposures and predicted effects in Puerto Rico, USA.

22. Hierarchy of signaling thresholds downstream of the T cell receptor and the Tec kinase ITK.

23. Genomic and Hormonal Biomarkers of Phthalate-Induced Male Rat Reproductive Developmental Toxicity Part II: A Targeted RT-qPCR Array Approach That Defines a Unique Adverse Outcome Pathway.

24. The View from the Benches: Scientists' Perspectives on the Uses and Governance of Human Gene-Editing Research.

25. Public and private tapwater: Comparative analysis of contaminant exposure and potential risk, Cape Cod, Massachusetts, USA.

26. Human GPR17 missense variants identified in metabolic disease patients have distinct downstream signaling profiles.

27. In vitro effects-based method and water quality screening model for use in pre- and post-distribution treated waters.

28. Hexafluoropropylene oxide-dimer acid (HFPO-DA or GenX) alters maternal and fetal glucose and lipid metabolism and produces neonatal mortality, low birthweight, and hepatomegaly in the Sprague-Dawley rat.

29. A New Governance Approach to Regulating Human Genome Editing.

30. Quantification of the Uncertainties in Extrapolating From In Vitro Androgen Receptor Antagonism to In Vivo Hershberger Assay Endpoints and Adverse Reproductive Development in Male Rats.

31. Activation of the Tec Kinase ITK Controls Graded IRF4 Expression in Response to Variations in TCR Signal Strength.

32. Is Real-Time ELSI Realistic?

33. De Facto Water Reuse: Bioassay suite approach delivers depth and breadth in endocrine active compound detection.

34. TCR signaling: it's all about the numbers.

35. Gpr17 deficiency in POMC neurons ameliorates the metabolic derangements caused by long-term high-fat diet feeding.

37. Predictive Analysis Using Chemical-Gene Interaction Networks Consistent with Observed Endocrine Activity and Mutagenicity of U.S. Streams.

38. Detection of Osmotic Shock-Induced Extracellular Nucleotide Release with a Genetically Encoded Fluorescent Sensor of ADP and ATP.

39. A Conflicted Tale of Two Novel AR Antagonists In Vitro and In Vivo: Pyrifluquinazon Versus Bisphenol C.

40. Adverse Maternal, Fetal, and Postnatal Effects of Hexafluoropropylene Oxide Dimer Acid (GenX) from Oral Gestational Exposure in Sprague-Dawley Rats.

41. Is Enhancement the Price of Prevention in Human Gene Editing?

42. Peptide Antigen Concentration Modulates Digital NFAT1 Activation in Primary Mouse Naive CD8 + T Cells as Measured by Flow Cytometry of Isolated Cell Nuclei.

43. Mixed "Antiandrogenic" Chemicals at Low Individual Doses Produce Reproductive Tract Malformations in the Male Rat.

44. Validation of an automated counting procedure for phthalate-induced testicular multinucleated germ cells.

45. Multidomain Control Over TEC Kinase Activation State Tunes the T Cell Response.

46. Imaging extracellular ATP with a genetically-encoded, ratiometric fluorescent sensor.

47. Sulfate transport kinetics and toxicity are modulated by sodium in aquatic insects.

48. Occurrence and In Vitro Bioactivity of Estrogen, Androgen, and Glucocorticoid Compounds in a Nationwide Screen of United States Stream Waters.

49. Which Results to Return: Subjective Judgments in Selecting Medically Actionable Genes.

50. Molecular Modeling Evaluation of the Enantiomers of a Novel Adenylyl Cyclase 2 Inhibitor.

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