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首页> 美国卫生研究院文献>Frontiers in Systems Neuroscience >Expression and Function of Chemokines CXCL9-11 in Micturition Pathways in Cyclophosphamide (CYP)-Induced Cystitis and Somatic Sensitivity in Mice
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Expression and Function of Chemokines CXCL9-11 in Micturition Pathways in Cyclophosphamide (CYP)-Induced Cystitis and Somatic Sensitivity in Mice

机译:趋化因子CXCL9-11在环磷酰胺(CYP)诱导的膀胱炎的排尿途径中的表达和功能及小鼠的体细胞敏感性

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Changes in urinary bladder function and somatic sensation may be mediated, in part, by inflammatory changes in the urinary bladder including the expression of chemokines. Male and female C57BL/6 mice were treated with cyclophosphamide (CYP; 75 mg/kg, 200 mg/kg, i.p.) to induce bladder inflammation (4 h, 48 h, chronic). We characterized the expression of CXC chemokines (CXCL9, CXCL10 and CXCL11) in the urinary bladder and determined the effects of blockade of their common receptor, CXCR3, at the level urinary bladder on bladder function and somatic (hindpaw and pelvic) sensation. qRT-PCR and Enzyme-Linked Immunoassays (ELISAs) were used to determine mRNA and protein expression of CXCL9, CXCL10 and CXCL11 in urothelium and detrusor. In urothelium of female mice treated with CYP, CXCL9 and CXCL10 mRNA significantly (p ≤ 0.01) increased with CYP treatment whereas CXC mRNA expression in the detrusor exhibited both increases and decreases in expression with CYP treatment. CXC mRNA expression urothelium and detrusor of male mice was more variable with both significant (p ≤ 0.01) increases and decreases in expression depending on the specific CXC chemokine and CYP treatment. CXCL9 and CXCL10 protein expression was significantly (p ≤ 0.01) increased in the urinary bladder with 4 h CYP treatment in female mice whereas CXC protein expression in the urinary bladder of male mice did not exhibit an overall change in expression. CXCR3 blockade with intravesical instillation of AMG487 (5 mg/kg) significantly (p ≤ 0.01) increased bladder capacity, reduced voiding frequency and reduced non-voiding contractions in female mice treated with CYP (4 h, 48 h). CXCR3 blockade also reduced (p ≤ 0.01) hindpaw and pelvic sensitivity in female mice treated with CYP (4 h, 48 h). CXC chemokines may be novel targets for treating urinary bladder dysfunction and somatic sensitization resulting from urinary bladder inflammation.
机译:膀胱功能的变化和躯体感觉的改变可能部分由膀胱中的炎症变化(包括趋化因子的表达)介导。将雄性和雌性C57BL / 6小鼠用环磷酰胺(CYP; 75 mg / kg,200 mg / kg,腹腔注射)治疗,以诱导膀胱炎症(4小时,48小时,慢性)。我们表征了CXC趋化因子(CXCL9,CXCL10和CXCL11)在膀胱中的表达,并确定了在膀胱水平上其共同受体CXCR3的阻断对膀胱功能和躯体(后爪和骨盆)感觉的影响。使用qRT-PCR和酶联免疫测定(ELISA)测定尿路上皮和逼尿肌中CXCL9,CXCL10和CXCL11的mRNA和蛋白表达。在用CYP处理的雌性小鼠的尿路上皮中,CXCL9和CXCL10 mRNA随CYP处理而显着增加(p≤0.01),而逼尿肌中CXC mRNA的表达随CYP处理而显示出增加和减少。雄性小鼠的CXC mRNA表达尿路上皮和逼尿肌更具可变性,根据特定的CXC趋化因子和CYP处理,表达均显着(p≤0.01)增加和减少。在雌性小鼠中,经4 h CYP处理后,膀胱中的CXCL9和CXCL10蛋白表达显着增加(p≤0.01),而雄性小鼠的膀胱中CXC蛋白表达没有整体表达变化。膀胱灌注AMG487(5 mg / kg)对CXCR3的阻滞作用(p≤0.01)显着(p≤0.01)增强了用CYP治疗的雌性小鼠的膀胱容量,减少的排尿频率和减少的非排空收缩(4 h,48 h)。在用CYP处理的雌性小鼠中(4 h,48 h),CXCR3阻滞也降低了(p≤0.01)后爪和骨盆敏感性。 CXC趋化因子可能是治疗膀胱功能障碍和膀胱炎症引起的体敏的新型靶标。

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