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1. Transcriptomic Analysis of Postnatal Rat Carotid Body Development

2. Intermittent hypoxia inhibits epinephrine-induced transcriptional changes in human aortic endothelial cells

3. Gasotransmitter modulation of hypoglossal motoneuron activity

4. The Roles of Morphology and Environment on the Star Formation Rate–Stellar Mass Relation in COSMOS from 0 < z < 3.5

5. Intermittent Hypoxia-Induced Activation of Endothelial Cells Is Mediated via Sympathetic Activation-Dependent Catecholamine Release

6. Histone Deacetylase 5 Is an Early Epigenetic Regulator of Intermittent Hypoxia Induced Sympathetic Nerve Activation and Blood Pressure

7. Recent advances in understanding the physiology of hypoxic sensing by the carotid body [version 1; referees: 2 approved]

9. Carotid Body O2 Sensing requires H2S-dependent Persulfidation of Olfactory Receptor 78

10. Adenylate Cyclase 3 and Cyclic Nucleotide-Gated Channel Alpha 2 Are Downstream Signaling to H2S/Olfr78 to Carotid Body Responses to Hypoxia

11. Recent advances in understanding the physiology of hypoxic sensing by the carotid body [version 1; peer review: 3 approved]

13. Hypoxia sensing requires H2S-dependent persulfidation of olfactory receptor 78.

14. A pleiotropic hypoxia-sensitive EPAS1 enhancer is disrupted by adaptive alleles in Tibetans

15. Homeostatic responses to hypoxia by the carotid body and adrenal medulla are based on mutual antagonism between HIF-1α and HIF-2α

16. Role of olfactory receptor78 in carotid body-dependent sympathetic activation and hypertension in murine models of chronic intermittent hypoxia

18. Carotid body responses to O

24. Adaptive cardiorespiratory changes to chronic continuous and intermittent hypoxia

25. Gasotransmitter modulation of hypoglossal motoneuron activity.

26. Olfactory receptor 78 participates in carotid body response to a wide range of low O2 levels but not severe hypoxia

27. Long-term facilitation of catecholamine secretion from adrenal chromaffin cells of neonatal rats by chronic intermittent hypoxia

28. The stellar mass versus stellar metallicity relation of star-forming galaxies at $1.6\le z\le3.0$ and implications for the evolution of the $\alpha$-enhancement

29. Esophageal Liposarcoma of the Oropharyngeal-Esophageal Junction.

30. Histone Deacetylase 5 Is an Early Epigenetic Regulator of Intermittent Hypoxia Induced Sympathetic Nerve Activation and Blood Pressure

31. H2S mediates carotid body response to hypoxia but not anoxia

32. Gaseous transmitter regulation of hypoxia-evoked catecholamine secretion from murine adrenal chromaffin cells

33. Olfactory receptor 78 regulates erythropoietin and cardiorespiratory responses to hypobaric hypoxia

34. Olfactory receptor 78 participates in carotid body response to a wide range of low O

35. DNA methylation in the central and efferent limbs of the chemoreflex requires carotid body neural activity

36. Epigenetic regulation of redox state mediates persistent cardiorespiratory abnormalities after long-term intermittent hypoxia

37. Neural Activation of Molecular Circuitry in Intermittent Hypoxia

38. Impaired carotid body hypoxic sensing in mice deficient in olfactory receptor 78

39. Phrenic Nerve and Carotid Body Responses to Hypoxia and CO 2 in Naked Mole Rats

41. Impaired Acute Hypoxic Sensing in Olfactory Receptor 78 Knockout Mice

42. H 2 S Contributes to Carotid Body Response to Hypoxia but Not Anoxia

43. Therapeutic Targeting of the Carotid Body for Treating Sleep Apnea in a Pre-clinical Mouse Model

44. Role of olfactory receptor78 in carotid body-dependent sympathetic activation and hypertension in murine models of chronic intermittent hypoxia.

45. Gaseous transmitter regulation of hypoxia-evoked catecholamine secretion from murine adrenal chromaffin cells.

46. Olfactory receptor 78 regulates erythropoietin and cardiorespiratory responses to hypobaric hypoxia.

47. H

48. REACTIVE OXYGEN RADICALS AND GASEOUS TRANSMITTERS IN THE CAROTID BODY ACTIVATION BY INTERMITTENT HYPOXIA

49. Measurement of Sensory Nerve Activity from the Carotid Body

50. Therapeutic Targeting of the Carotid Body for Treating Sleep Apnea in a Pre-clinical Mouse Model

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