INT108348

Context	Info
Confidence	0.68
First Reported	2003
Last Reported	2010
Negated	1
Speculated	0
Reported most in	Body
Documents	10
Total Number	10
Disease Relevance	4.94
Pain Relevance	0.82

This is a graph with borders and nodes. Maybe there is an Imagemap used so the nodes may be linking to some Pages.

aging (Aqp2)	plasma membrane (Aqp2)	protein complex (Aqp2)
transmembrane transport (Aqp2)	lysosome (Aqp2)	cytoplasm (Aqp2)

Anatomy Link	Frequency
urine	6
plasma	1
lumen	1

Aqp2 (Rattus norvegicus)

Pain Link	Frequency	Relevance
COX-2 inhibitor	10	99.54
cINOD	8	96.20
ischemia	11	92.04
medulla	4	56.24
anesthesia	15	50.00
antagonist	20	5.00
isoflurane	16	5.00
Inflammation	11	5.00
withdrawal	6	5.00
alcohol	4	5.00

Disease Link	Frequency	Relevance
Polyuria	13	99.90
Diabetes Insipidus	20	99.56
Cv Unclassified Under Development	8	92.04
INFLAMMATION	17	91.20
Injury	31	85.04
Chronic Renal Failure	522	83.32
Pressure And Volume Under Development	17	82.60
Reperfusion Injury	3	76.24
Renal Disease	23	66.16
Body Weight	10	60.80

Sentences Mentioned In

Key:

Protein

Mutation

Event

Anatomy

Negation

Speculation

Pain term

Disease term

Treating lithium-induced nephrogenic diabetes insipidus with a COX-2 inhibitor improves polyuria via upregulation of AQP2 and NKCC2.

Positive_regulation (upregulation) of AQP2 associated with polyuria, diabetes insipidus and cox-2 inhibitor

1)	Confidence	0.68	Published	2008	Journal	Am. J. Physiol. Renal Physiol.	Section	Title	Doc Link	18216147	Disease Relevance	0.74	Pain Relevance	0.33

Baseline urine osmolality was greater in the TD group than in the control and the TT groups, an effect associated with increased renal aquaporin 2 level.

Positive_regulation (increased) of aquaporin 2 in urine

2)	Confidence	0.66	Published	2010	Journal	J Biomed Sci	Section	Abstract	Doc Link	PMC2994366	Disease Relevance	0.33	Pain Relevance	0.08

The upregulation of AQP2 and NKCC2 in response to the COX-2 inhibitor may underlie the therapeutic mechanisms by which NSAIDs enhance antidiuresis in patients with NDI.

Positive_regulation (upregulation) of AQP2 associated with diabetes insipidus, cinod and cox-2 inhibitor

3)	Confidence	0.49	Published	2008	Journal	Am. J. Physiol. Renal Physiol.	Section	Abstract	Doc Link	18216147	Disease Relevance	0.73	Pain Relevance	0.30

Interestingly, in a parallel study, we found that treatment with the AT1 receptor blocker candesartan in NaCl-restricted normal rats prevented the increase of the expression of inner medullary AQP2 and phosphorylated-AQP2 (AQP2 phosphorylated in the PKA-phosphorylation consensus site Ser-256) and the increase of urine concentration in response to the long-term dDAVP treatment (25).

Positive_regulation (increase) of AQP2 in urine

4)	Confidence	0.47	Published	2005	Journal	Journal of Korean Medical Science	Section	Body	Doc Link	PMC2808601	Disease Relevance	0.69	Pain Relevance	0.03

Interestingly, in a parallel study, we found that treatment with the AT1 receptor blocker candesartan in NaCl-restricted normal rats prevented the increase of the expression of inner medullary AQP2 and phosphorylated-AQP2 (AQP2 phosphorylated in the PKA-phosphorylation consensus site Ser-256) and the increase of urine concentration in response to the long-term dDAVP treatment (25).

Positive_regulation (increase) of AQP2 in urine

5)	Confidence	0.47	Published	2005	Journal	Journal of Korean Medical Science	Section	Body	Doc Link	PMC2808601	Disease Relevance	0.70	Pain Relevance	0.03

Interestingly, in a parallel study, we found that treatment with the AT1 receptor blocker candesartan in NaCl-restricted normal rats prevented the increase of the expression of inner medullary AQP2 and phosphorylated-AQP2 (AQP2 phosphorylated in the PKA-phosphorylation consensus site Ser-256) and the increase of urine concentration in response to the long-term dDAVP treatment (25).

Positive_regulation (increase) of AQP2 in urine

6)	Confidence	0.47	Published	2005	Journal	Journal of Korean Medical Science	Section	Body	Doc Link	PMC2808601	Disease Relevance	0.69	Pain Relevance	0.03

Interestingly, in a parallel study, we found that treatment with the AT1 receptor blocker candesartan in NaCl-restricted normal rats prevented the increase of the expression of inner medullary AQP2 and phosphorylated-AQP2 (AQP2 phosphorylated in the PKA-phosphorylation consensus site Ser-256) and the increase of urine concentration in response to the long-term dDAVP treatment (25).

Positive_regulation (increase) of AQP2 in urine

7)	Confidence	0.41	Published	2005	Journal	Journal of Korean Medical Science	Section	Body	Doc Link	PMC2808601	Disease Relevance	0.68	Pain Relevance	0.03

The concentration of AQP2 was not significantly changed during the urine concentrating test in Groups 3 and 4, but increased significantly in the other two groups.

Neg (not) Positive_regulation (increased) of AQP2 in urine

8)	Confidence	0.36	Published	2010	Journal	BMC Nephrol	Section	Body	Doc Link	PMC2965705	Disease Relevance	0.07	Pain Relevance	0

This results in an increased production of c-AMP, which through a cascade of intracellular reactions upregulate the AQP 2 water channels, and thereby promotes water transport from the tubular lumen to the cell.

Positive_regulation (upregulate) of AQP 2 in lumen

9)	Confidence	0.29	Published	2010	Journal	BMC Nephrol	Section	Body	Doc Link	PMC2965705	Disease Relevance	0.30	Pain Relevance	0

RESULTS: Increases in plasma AM levels were observed in parallel with increases in the levels of urinary AQP2/creatinine (Cr) before induction and 90 and 180 min after initiation of anesthesia.

Positive_regulation (increases) of AQP2 in plasma

10)	Confidence	0.14	Published	2003	Journal	Horm. Res.	Section	Body	Doc Link	12566732	Disease Relevance	0	Pain Relevance	0

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INT108348

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