Abstract Background Curcumin has anti-inflammatory, anti-oxidant, and anti-proliferative properties, and depending upon the experimental circumstances, may be pro- or anti-apoptotic. Many of these biological actions could ameliorate diabetic nephropathy. Methods/Design Mouse podocytes, cultured in basal or high glucose conditions, underwent acute exposure to curcumin. Western blots for p38-MAPK, COX-2 and cleaved caspase-3; isoelectric focusing for HSP25 phosphorylation; and DNase I assays for F- to G- actin cleavage were performed for <it>in vitro </it>analyses. <it>In vivo </it>studies examined the effects of dietary curcumin on the development of diabetic nephropathy in streptozotocin (Stz)-induced diabetes in DBA2J mice. Urinary albumin to creatinine ratios were obtained, high performance liquid chromatography was performed for urinary curcuminoid measurements, and Western blots for p38-MAPK and total HSP25 were performed. Results Curcumin enhanced the phosphorylation of both p38MAPK and downstream HSP25; inhibited COX-2; induced a trend towards attenuation of F- to G-actin cleavage; and dramatically inhibited the activation of caspase-3 in <it>vitro</it>. In curcumin-treated DBA2J mice with Stz-diabetes, HPLC measurements confirmed the presence of urinary curcuminoid. Nevertheless, dietary provision of curcumin either before or after the induction of diabetes failed to attenuate albuminuria. Conclusions Apart from species, strain, early differences in glycemic control, and/or dosing effects, the failure to modulate albuminuria may have been due to a decrement in renal HSP25 or stimulation of the 12/15 lipoxygenase pathway in DBA2J mice fed curcumin. In addition, these studies suggest that timed urine collections may be useful for monitoring curcumin dosing and renal pharmacodynamic effects.</p

A Goel

A Hall

A Minden

A Parcellier

A Scharstuhl

A Schieppati

A Sood

A Ukil

AJ Macario

B Isermann

B Li

BT Kurien

C Kubisch

C Paul

C Schafer

C Selvam

CT Okamoto

CV Rao

CW Gourlay

D Karunagaran

DD Heath

E Skrzypczak-Jankun

E Tourkina

EA Papakonstanti

F Zhang

G Began

G Kang

GP Lim

HE Lee

I Antonipillai

I Blikstad

J Chiu

J Dujic

J Guay

J Holy

J Huot

J Ma

Janine LaPage

JC Shu

JH Woo

JL Watson

JM Bruey

JN Lavoie

Jun Ma

JW Cho

K Kato

K Tikoo

KE Dunsmore

KJ Park

KN Bitar

KS Chun

Lynetta Phillips

M Hu

M Singh

MA Bill

MA Reddy

ME Dunlop

MH Meyer

MT Huang

N Raman

NM Weir

OA Coso

P Mehlen

P Mundel

PS Babu

Q Chen

QY Chen

R Li

R Natarajan

Rama Natarajan

S Pichon

S Priya

S Reuter

S Sharma

SAaKAE Loktionova

SB Brown

Sharon G Adler

SJ Lim

SK Van Why

SW Kang

T Dai

T Mashima

T Zarubin

Tiane Dai

TW Owens

U Knauf

W Hartojo

WE Smoyer

WH Chan

X Preville

X Song

X Zhang

YC Chen

YD Hsuuw

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A 12-lipoxygenase product, 12-hydroxyeicosatetraenoic acid, is increased in diabetics with incipient and early renal disease.

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JS: The melanoma-associated transmembrane glycoprotein Gpnmb controls trafficking of cellular debris for degradation and is essential for tissue repair.

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Stress- and mitogeninduced phosphorylation of the small heat shock protein Hsp25 by MAPKAP kinase 2 is not essential for chaperone properties and cellular thermoresistance.

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Curcumin activates the p38MPAK-HSP25 pathway in vitro but fails to attenuate diabetic nephropathy in DBA2J mice despite urinary clearance documented by HPLC