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1. Altered Tau Kinase Activity in rTg4510 Mice after a Single Interfaced CHIMERA Traumatic Brain Injury

2. An in vitro bioengineered model of the human arterial neurovascular unit to study neurodegenerative diseases

3. Axl receptor tyrosine kinase is a regulator of apolipoprotein E

4. ApoA-I deficiency increases cortical amyloid deposition, cerebral amyloid angiopathy, cortical and hippocampal astrogliosis, and amyloid-associated astrocyte reactivity in APP/PS1 mice

5. Small molecule inducers of ABCA1 and apoE that act through indirect activation of the LXR pathway

6. Hormonal modulators of glial ABCA1 and apoE levels[S]

7. ABCA1 influences neuroinflammation and neuronal death

8. Identification of a Chrysanthemic Ester as an Apolipoprotein E Inducer in Astrocytes.

9. An ABCA1-independent pathway for recycling a poorly lipidated 8.1 nm apolipoprotein E particle from glia

10. LCAT synthesized by primary astrocytes esterifies cholesterol on glia-derived lipoproteins

11. ABCG1 influences the brain cholesterol biosynthetic pathway but does not affect amyloid precursor protein or apolipoprotein E metabolism in vivo

12. Physiologically regulated transgenic ABCA1 does not reduce amyloid burden or amyloid-β peptide levels in vivo

13. The liver X receptor agonist GW3965 improves recovery from mild repetitive traumatic brain injury in mice partly through apolipoprotein E.

14. LEVERAGING THE POWER OF 3D BRAIN-WIDE IMAGING AND MAPPING TOOLS FOR BRAIN INJURY RESEARCH IN MURINE MODELS

15. Altered tau in rTg4510 mice after a single interfaced CHIMERA traumatic brain injury

16. HDL from an Alzheimer's disease perspective

17. The effects of peripheral lipoprotein metabolism on cerebrovascular inflammation in APP/PS1 mice

18. An in vitro bioengineered model of the human arterial neurovascular unit to study neurodegenerative diseases

19. Axl receptor tyrosine kinase is a regulator of apolipoprotein E

20. Additional file 3 of An in vitro bioengineered model of the human arterial neurovascular unit to study neurodegenerative diseases

21. Additional file 2 of An in vitro bioengineered model of the human arterial neurovascular unit to study neurodegenerative diseases

22. Additional file 1 of An in vitro bioengineered model of the human arterial neurovascular unit to study neurodegenerative diseases

23. Additional file 4 of An in vitro bioengineered model of the human arterial neurovascular unit to study neurodegenerative diseases

24. Small molecule inducers of ABCA1 and apoE that act through indirect activation of the LXR pathway

25. Additional file 2: of ApoA-I deficiency increases cortical amyloid deposition, cerebral amyloid angiopathy, cortical and hippocampal astrogliosis, and amyloid-associated astrocyte reactivity in APP/PS1 mice

26. Additional file 1: of ApoA-I deficiency increases cortical amyloid deposition, cerebral amyloid angiopathy, cortical and hippocampal astrogliosis, and amyloid-associated astrocyte reactivity in APP/PS1 mice

27. P4-164: APOA-I DEFICIENCY INCREASES CORTICAL AMYLOID DEPOSITION, CEREBRAL AMYLOID ANGIOPATHY, CORTICAL AND HIPPOCAMPAL ASTROGLIOSIS AND AMYLOID-ASSOCIATED ASTROCYTE REACTIVITY IN APP/PS1 MICE

28. Hormonal modulators of glial ABCA1 and apoE levels[S]

29. ABCA1 influences neuroinflammation and neuronal death

30. An ABCA1-independent pathway for recycling a poorly lipidated 8.1 nm apolipoprotein E particle from glia

31. ATP-binding Cassette Transporter A1 Mediates the Beneficial Effects of the Liver X Receptor Agonist GW3965 on Object Recognition Memory and Amyloid Burden in Amyloid Precursor Protein/Presenilin 1 Mice*

32. Greasing the wheels of Aβ clearance in Alzheimer's Disease: The role of lipids and apolipoprotein E

33. Overexpression of Human ABCG1 Does Not Affect Atherosclerosis in Fat-Fed ApoE-Deficient Mice

34. Physiologically regulated transgenic ABCA1 does not reduce amyloid burden or amyloid-β peptide levels in vivo

35. Reconstituted high-density lipoproteins acutely reduce soluble brain Aβ levels in symptomatic APP/PS1 mice

36. Intravenously Injected Human Apolipoprotein A‐I Rapidly Enters the Central Nervous System via the Choroid Plexus

37. P1‐006: INTRAVENOUSLY INJECTED HUMAN APOLIPOPROTEIN A‐I RAPIDLY ENTERS THE CENTRAL NERVOUS SYSTEM VIA THE CHOROID PLEXUS IN MICE

38. Abstract 245: Intravenously Injected Human Apolipoprotein A-I Rapidly Enters the Central Nervous System via the Choroid Plexus in Mice

39. The Liver X Receptor Agonist GW3965 Improves Recovery from Mild Repetitive Traumatic Brain Injury in Mice Partly through Apolipoprotein E

40. Identification of a Chrysanthemic Ester as an Apolipoprotein E Inducer in Astrocytes

41. P4‐218: The liver X receptor agonist GW3965 improves cognitive deficits, reduces beta‐amyloid elevation and suppresses neuronal damage following mild repetitive closed head injury in mice

42. P1‐258: ABCA1 mediates the beneficial effects of the liver‐X‐receptor agonist GW3965 on amyloid load and object recognition memory in APP/PS1 Alzheimer mice

43. Cholesterol defect is marked across multiple rodent models of Huntington's disease and is manifest in astrocytes

44. P2‐150: Lecithin: Cholesterol Acyltransferase (LCAT) is required for normal brain apoE metabolism in mice

45. LCAT synthesized by primary astrocytes esterifies cholesterol on glia-derived lipoproteins

46. Specific loss of brain ABCA1 increases brain cholesterol uptake and influences neuronal structure and function

47. P4‐313: The effects of Gw3965 on the neuropathological and cognitive outcome in the APP/PS1 model of Alzheimer's disease with and without ABCA1

48. ABCG1 influences the brain cholesterol biosynthetic pathway but does not affect amyloid precursor protein or apolipoprotein E metabolism in vivo

49. Merging pathology with biomechanics using CHIMERA (Closed-Head Impact Model of Engineered Rotational Acceleration): a novel, surgery-free model of traumatic brain injury.

50. Cholesterol Defect Is Marked across Multiple Rodent Models of Huntington's Disease and Is Manifest in Astrocytes.

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