Improved Effects of Viral Gene Delivery of Human uPA plus Biliodigestive Anastomosis Induce Recovery from Experimental Biliary Cirrhosis

Miranda-Díaz, Alejandra Guillermina; Rincón, Ana Rosa; Salgado, Silvia; Vera-Cruz, José María; Villafuerte-Gálvez, Javier; Islas, Ma Cristina; Berumen, Jaime; Aguilar-Córdova, Estuardo; Armendáriz‐Borunda, Juan

doi:10.1016/j.ymthe.2003.09.015

Cited by 13 publications

(13 citation statements)

References 27 publications

(31 reference statements)

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“…uPA also requires additional factors like binding to uPAR for optimal activity,48, 49 and therefore might have a different spatial and temporal activity pattern than tPA even though liver homogenates have comparable enzymatic activity for both proteases after BDL. While the role of uPA after BDL remains uncertain,50 our data demonstrate that uPA cannot substitute for tPA in this setting. Furthermore, the ability to reverse the effects of PAI‐1 deficiency on BDL‐induced liver injury using tPA‐STOP provides strong suggestive but not conclusive evidence that the protective effects of PAI‐1 deficiency are primarily mediated by increased tPA, and not uPA, activity.…”

Section: Discussionmentioning

confidence: 62%

Tissue-type plasminogen activator deficiency exacerbates cholestatic liver injury in mice

2007

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Recent studies demonstrating a role for plasminogen activator inhibitor (PAI)-1 in cholestatic liver disease in mice suggested that tissue-type plasminogen activator (tPA) or urokinase plasminogen activator (uPA) might be important after biliary tract obstruction. We now demonstrate that blocking tPA exacerbates liver injury after bile duct ligation (BDL). tPA deficient mice have increased bile infarcts, increased TUNEL positive cells, increased neutrophil infiltration, reduced hepatocyte proliferation and reduced ductular reaction 72 hours after BDL compared to wild type mice. In addition, the protective and proliferative effects of plasminogen activator inhibitor 1 (PAI-1) deficiency after BDL are dramatically blocked by the tPA inhibitor tPA-STOP. One potential mechanism for these effects is that both tPA deficiency and tPA-STOP reduce hepatocyte growth factor (HGF) activation and c-Met phosphorylation in the liver after BDL. In support of this hypothesis, HGF treatment reverses the effects of tPA deficiency in mice. Furthermore, preferential tPA activation in areas of injury after BDL might occur because fibrin accumulates in bile infarcts and activates tPA. Conclusion: tPA inactivation accelerates liver injury after BDL and reduces HGF activation. These data suggest that strategies to increase HGF activation might be protective in liver diseases with biliary tract obstruction even without increased HGF production.

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Section: Discussionmentioning

confidence: 62%

Tissue-type plasminogen activator deficiency exacerbates cholestatic liver injury in mice

2007

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“…Several MMPs and growth factors have been suggested to contribute to this effect [85,[101][102][103][104]. Thus, declining TIMP-1 levels may lead to an increase in MMP activity thereby exerting two effects: (i) degradation of ECM to allow hepatocyte expansion and (ii) release of ECM-bound pro-HGF (hepatocyte growth factor).…”

Section: Mmps and Timps In Fibrolysismentioning

confidence: 99%

Expression of MMPs and TIMPs in liver fibrosis – a systematic review with special emphasis on anti-fibrotic strategies

Hemmann

Graf

Roderfeld

et al. 2007

Journal of Hepatology

441

348

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“…However, they do not clarify the role of endogenous renal uPA during fibrogenesis. Results from other experimental model systems fail to answer this question, as uPA has been reported to promote or attenuate fibrosis, depending on the organ and disease model that is investigated (2,7,9,13,18,21,26,27). To determine the role of uPA in the pathogenesis of chronic renal interstitial fibrosis, disease severity in response to UUO was compared between WT and uPAϪ/Ϫ mice.…”

mentioning

confidence: 99%

Endogenous urokinase lacks antifibrotic activity during progressive renal injury

Yamaguchi¹,

López-Guisa²,

Cai³

et al. 2007

American Journal of Physiology-Renal Physiology

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Interstitial fibrosis is a universal feature of progressive kidney disease. Urokinase-type plasminogen activator (uPA) is thought to participate for several reasons: 1) uPA is produced predominantly in kidney, 2) its inhibitor plasminogen activator inhibitor-1 (PAI-1) is a strong promoter of interstitial fibrosis, whereas its receptor (uPAR) attenuates renal fibrosis, 3) uPA reduces fibrosis in liver and lung, and 4) uPA can activate hepatocyte growth factor (HGF), a potent antifibrotic growth factor. The present study tested the hypothesis that endogenous uPA reduces fibrosis severity by investigating the unilateral ureteral obstruction (UUO) model in wild-type (WT) and uPA-/- mice. Several outcomes were measured: renal collagen 3-21 days after UUO, macrophage accumulation (F4/80 Western blotting), interstitial myofibroblast density (alpha-smooth muscle actin immunostaining), and tubular injury (E-cadherin and Ksp-cadherin Western blotting). None of these measures differed significantly between WT and uPA-/- mice. uPA genetic deficiency was not associated with compensatory changes in renal uPAR mRNA levels, PAI-1 protein levels, or tissue plasminogen activator activity levels after UUO. Despite the known ability of uPA to activate latent HGF, immunoblotting failed to detect significant differences in levels of the active HGF alpha-chain and phosphorylated cMET (the activated HGF receptor) between the WT and uPA-/- groups. These findings suggest that the profibrotic actions of PAI-1 are uPA independent and that an alternative pathway must activate HGF in kidney. Finally, these results highlight a significant organ-specific difference in basic fibrogenic pathways, as enhanced uPA activity has been reported to attenuate pulmonary and hepatic fibrosis.

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Improved Effects of Viral Gene Delivery of Human uPA plus Biliodigestive Anastomosis Induce Recovery from Experimental Biliary Cirrhosis

Cited by 13 publications

References 27 publications

Tissue-type plasminogen activator deficiency exacerbates cholestatic liver injury in mice

Tissue-type plasminogen activator deficiency exacerbates cholestatic liver injury in mice

Expression of MMPs and TIMPs in liver fibrosis – a systematic review with special emphasis on anti-fibrotic strategies

Endogenous urokinase lacks antifibrotic activity during progressive renal injury

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