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Renin Inhibition Improves Cardiac Function and Remodeling After Myocardial Infarction Independent of Blood Pressure

Westermann, Dirk ; Riad, Alexander ; Lettau, Olga ; [et al.]

Ovid Technologies (Wolters Kluwer Health) ; 2008

In: Hypertension Vol. 52, No. 6 ( 2008-12), p. 1068-1075

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In: Hypertension, Ovid Technologies (Wolters Kluwer Health), Vol. 52, No. 6 ( 2008-12), p. 1068-1075

Abstract: Pharmacological renin inhibition with aliskiren is an effective antihypertensive drug treatment, but it is currently unknown whether aliskiren is able to attenuate cardiac failure independent of its blood pressure–lowering effects. We investigated the effect of aliskiren on cardiac remodeling, apoptosis, and left ventricular (LV) function after experimental myocardial infarction (MI). C57J/bl6 mice were subjected to coronary artery ligation and were treated for 10 days with vehicle or aliskiren (50 mg/kg per day via an SC osmopump), whereas sham-operated animals served as controls. This dose of aliskiren, which did not affect systemic blood pressure, improved systolic and diastolic LV function, as measured by the assessment of pressure-volume loops after MI. Furthermore, after MI LV dilatation, cardiac hypertrophy and lung weights were decreased in mice treated with aliskiren compared with placebo-treated mice after MI. This was associated with a normalization of the mitogen-activated protein kinase P38 and extracellular signal-regulated kinases 1/2, AKT, and the apoptotic markers bax and bcl-2 (all measured by Western blots), as well as the number of TUNEL-positive cells in histology. LV dilatation, as well as the associated upregulation of gene expression (mRNA abundance) and activity (by zymography) of the cardiac metalloproteinase 9 in the placebo group after MI, was also attenuated in the aliskiren-treated group. Aliskiren improved LV dysfunction after MI in a dose that did not affect blood pressure. This was associated with the amelioration of cardiac remodelling, hypertrophy, and apoptosis.

Type of Medium: Online Resource

ISSN: 0194-911X , 1524-4563

URL: Article

DOI: 10.1161/HYPERTENSIONAHA.108.116350

Language: English

Publisher: Ovid Technologies (Wolters Kluwer Health)

Publication Date: 2008

detail.hit.zdb_id: 2094210-2

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Doxorubicin cardiomyopathy-induced inflammation and apoptosis are attenuated by gene deletion of the kinin B1 receptor

Westermann, Dirk ; Lettau, Olga ; Sobirey, Meike ; [et al.]

Walter de Gruyter GmbH ; 2008

In: bchm Vol. 389, No. 6 ( 2008-06-01), p. 713-718

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In: bchm, Walter de Gruyter GmbH, Vol. 389, No. 6 ( 2008-06-01), p. 713-718

Abstract: Clinical use of the anthracycline doxorubicin (DOX) is limited by its cardiotoxic effects, which are attributed to the induction of apoptosis. To elucidate the possible role of the kinin B1 receptor (B1R) during the development of DOX cardiomyopathy, we studied B1R knockout mice (B1R -/- ) by investigating cardiac inflammation and apoptosis after induction of DOX-induced cardiomyopathy. DOX control mice showed cardiac dysfunction measured by pressure-volume loops in vivo . This was associated with a reduced activation state of AKT, as well as an increased bax/bcl2 ratio in Western blots, indicating cardiac apoptosis. Furthermore, mRNA levels of the proinflammatory cytokine interleukin 6 were increased in the cardiac tissue. In DOX B1R -/- mice, cardiac dysfunction was improved compared to DOX control mice, which was associated with normalization of the bax/bcl-2 ratio and interleukin 6, as well as AKT activation state. These findings suggest that B1R is detrimental in DOX cardiomyopathy in that it mediates the inflammatory response and apoptosis. These insights might have useful implications for future studies utilizing B1R antagonists for treatment of human DOX cardiomyopathy.

Type of Medium: Online Resource

ISSN: 1437-4315 , 1431-6730

URL: Article

DOI: 10.1515/BC.2008.070

Language: English

Publisher: Walter de Gruyter GmbH

Publication Date: 2008

detail.hit.zdb_id: 1466062-3

SSG: 12

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Myeloid differentiation factor-88 contributes to TLR9-mediated modulation of acute coxsackievirus B3-induced myocarditis in vivo

Riad, Alexander ; Westermann, Dirk ; Escher, Felicitas ; [et al.]

American Physiological Society ; 2010

In: American Journal of Physiology-Heart and Circulatory Physiology Vol. 298, No. 6 ( 2010-06), p. H2024-H2031

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In: American Journal of Physiology-Heart and Circulatory Physiology, American Physiological Society, Vol. 298, No. 6 ( 2010-06), p. H2024-H2031

Abstract: Toll-like receptor 9 (TLR9) is a member of the innate immune system and has been shown to influence myocardial function, but its role in myocarditis is hitherto unknown. We therefore investigated whether or not TLR9 plays a role in this disease in coxsackievirus B3 (CVB3)-induced myocarditis in mice. Left ventricular (LV) function, cardiac immune cell infiltration, virus mRNA, and components of the TLR9 downstream pathway were investigated in TLR9-deficient [knockout (KO)] and wild-type (WT) mice after infection with CVB3. Murine cardiac TLR9 expression was significantly increased in WT mice with acute CVB3 infection but not in WT mice with chronic myocarditis. Furthermore, in the acute phase of CVB3-induced myocarditis, CVB3-infected KO mice displayed improved LV function associated with reduced cardiac inflammation indexed by reduced amounts of immune cells compared with CVB3-infected WT mice. In contrast, in the chronic phase, LV function and inflammation were not seen to differ among the infected groups. The cardioprotective effects due to TLR9 deficiency were associated with suppression of the TLR9 downstream pathway as indexed by reduced cardiac levels of the adapter protein myeloid differentiation factor (MyD)-88 and the proinflammatory cytokine TNF-α. In addition, TLR9 deficiency led to an activation of the antiviral cytokine interferon-β in the heart as a result from viral infection. In conclusion, the MyD88/TNF-α axis due to TLR9 activation in the heart contributes the development of acute myocarditis but not of chronic myocarditis.

Type of Medium: Online Resource

ISSN: 0363-6135 , 1522-1539

URL: Article

DOI: 10.1152/ajpheart.01188.2009

RVK:

WA 15000

Language: English

Publisher: American Physiological Society

Publication Date: 2010

detail.hit.zdb_id: 1477308-9

SSG: 12

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TRIF Is a Critical Survival Factor in Viral Cardiomyopathy

Riad, Alexander ; Westermann, Dirk ; Zietsch, Christin ; [et al.]

The American Association of Immunologists ; 2011

In: The Journal of Immunology Vol. 186, No. 4 ( 2011-02-15), p. 2561-2570

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In: The Journal of Immunology, The American Association of Immunologists, Vol. 186, No. 4 ( 2011-02-15), p. 2561-2570

Abstract: TRIF is a member of the innate immune system known to be involved in viral recognition and type I IFN activation. Because IFNs are thought to play an important role in viral myocarditis, we investigated the role of TRIF in induced myocarditis in mice. Whereas C57BL/6 (wild-type) mice showed only mild myocarditis, including normal survival postinfection with coxsackievirus group B serotype 3 (CVB3), infection of TRIF−/− mice led to the induction of cardiac remodeling, severe heart failure, and 100% mortality (p & lt; 0.0001). These mice showed markedly reduced virus control in cardiac tissues and cardiomyocytes. This was accompained with dynamic cardiac cytokine activation in the heart, including a suppression of the antiviral cytokine IFN-β in the early viremic phase. TRIF−/− myocytes displayed a TLR4-dependent suppression of IFN-β, and pharmacological treatment of CVB3-infected TRIF−/− mice with murine IFN-β led to improved virus control and reduced cardiac inflammation. Additionally, this treatment within the viremic phase of myocarditis showed a significant long-term outcome indexed by reduced mortality (20 versus 100%; p & lt; 0.001). TRIF is essential toward a cardioprotection against CVB3 infection.

Type of Medium: Online Resource

ISSN: 0022-1767 , 1550-6606

URL: Article

DOI: 10.4049/jimmunol.1002029

RVK:

XA 54100

RVK:

XA 10000

Language: English

Publisher: The American Association of Immunologists

Publication Date: 2011

detail.hit.zdb_id: 1475085-5

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