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Increased cellular expression of matrix proteins that regulate mineralization is associated with calcification of native human and porcine xenograft bioprosthetic heart valves.

机译：调节矿化作用的基质蛋白的细胞表达增加与天然人和猪异种移植生物瓣膜的钙化有关。

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摘要

Dystrophic mineralization remains the leading cause of stenotic or regurgitant failure in native human and porcine bioprosthetic heart valves. We hypothesized that cellular expression of noncollagenous matrix proteins (osteopontin, osteocalcin, and osteonectin) that regulate skeletal mineralization may orchestrate valvular calcification. Porcine bioprosthetic heart valves and native human heart valves obtained during replacement surgery were analyzed for cells, matrix proteins that regulate mineralization, and vessels. Cell accumulation and calcification were correlated for both valve types (rho = 0.75, P = 0.01, native; rho = 0.42, P = 0.08, bioprosthetic). Osteopontin expression correlated with cell accumulation (rho = 0.58, P = 0.04) and calcification (rho = 0.52, P = 0.06) for bioprosthetic valves. Osteocalcin expression correlated with calcification (rho = 0.77, P = 0.04) and cell accumulation (rho = 0.69, P = 0.07) in native valves. Comparisons of calcified versus noncalcified native and bioprosthetic valves for averaged total matrix protein mRNA signal score revealed increased noncollagenous proteins mRNA levels in calcified valves (P = 0.07, group I vs. group II; P = 0.02, group III vs. group IV). When stratified according to positive versus negative mRNA signal status, both calcified bioprosthetic valves (P = 0.03) and calcified native valves (P = 0.01) were significantly more positive for noncollagenous proteins mRNA than their noncalcified counterparts. Local cell-associated expression of proteins regulating mineralization suggests a highly coordinated mechanism of bioprosthetic and native valve calcification analogous to physiologic bone mineralization. Modulation of cellular infiltration or cellular expression of matrix proteins that regulate mineralization, may offer an effective therapeutic approach to the prevention of valve failure secondary to calcification.

机译：营养不良的矿化仍然是天然人和猪生物人工心脏瓣膜狭窄或反流衰竭的主要原因。我们假设调节骨骼矿化作用的非胶原基质蛋白（骨桥蛋白，骨钙蛋白和骨连接蛋白）的细胞表达可能会导致瓣膜钙化。分析了置换手术期间获得的猪生物人工心脏瓣膜和天然人心脏瓣膜的细胞，调节矿化的基质蛋白和血管。两种瓣膜类型的细胞积累和钙化均相关（rho = 0.75，P = 0.01，天然； rho = 0.42，P = 0.08，生物修复）。骨桥蛋白的表达与生物瓣膜的细胞积累（rho = 0.58，P = 0.04）和钙化（rho = 0.52，P = 0.06）相关。骨钙蛋白的表达与天然瓣膜中的钙化（rho = 0.77，P = 0.04）和细胞蓄积（rho = 0.69，P = 0.07）相关。比较钙化和非钙化天然瓣膜和生物修复瓣膜的平均总基质蛋白mRNA信号得分，发现钙化瓣膜中非胶原蛋白mRNA水平增加（P = 0.07，I组vs. II组； P = 0.02，III组vs. IV组）。当根据阳性与阴性mRNA信号状态进行分层时，钙化生物假体瓣膜（P = 0.03）和钙化天然瓣膜（P = 0.01）相比非胶原蛋白mRNA的非胶原蛋白mRNA阳性显着更高。调节矿化的蛋白质的局部细胞相关表达表明，生物假体和天然瓣膜钙化的高度协调机制类似于生理性骨矿化。调节矿化作用的细胞浸润或基质蛋白的细胞表达调节可为预防继发于钙化的瓣膜衰竭提供有效的治疗方法。

著录项

期刊名称 The Journal of Clinical Investigation
作者
S S Srivatsa; P J Harrity; P B Maercklein; L Kleppe; J Veinot; W D Edwards; C M Johnson; L A Fitzpatrick;
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作者单位

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年(卷),期 1997(99),5
年度 1997
页码 996–1009
总页数 14
原文格式 PDF
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中图分类医学史;
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1. Physicochemical and microscopical study of calcific deposits from natural and bioprosthetic heart valves. Comparison and implications for mineralization mechanism [J] . D. MIKROULIS, D. MAVRILAS, J. KAPOLOS, Journal of Materials Science. Materials in Medicine . 2002,第9期

机译：天然和生物人工心脏瓣膜钙化沉积物的物理化学和微观研究。矿化机理的比较及启示
2. Matrix metalloproteinases in human melanoma cell lines and xenografts: increased expression of activated matrix metalloproteinase-2 (MMP-2) correlates with melanoma progression [J] . British Journal of Cancer . 1999,第5期

机译：人黑素瘤细胞系和异种移植物中的基质金属蛋白酶：激活的基质金属蛋白酶2（MMP-2）的表达增加与黑色素瘤的进展有关
3. Comparative study of cellular and extracellular matrix composition of native and tissue engineered heart valves. [J] . Schenke Layland K, Riemann I, Opitz F, Matrix biology: Journal of the International Society for Matrix Biology . 2004,第2期

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4. Extracellular Matrix Proteins Regulate Heart Valve Calcification [C] . Kathleen M. Reed, Karien J. Rodriguez, Kristyn S. Masters Society for Biomaterials Transaction Annual Meeting vol.29 pt.1 . 2006

机译：细胞外基质蛋白调节心脏瓣膜钙化
5. Extracellular Matrix Engineering of Porcine Bioprosthetic Heart Valves [D] . Petrovic, Mark Ian. 2021

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6. Matrix metalloproteinases in human melanoma cell lines and xenografts: increased expression of activated matrix metalloproteinase-2 (MMP-2) correlates with melanoma progression [O] . U B Hofmann, J R Westphal, E T Waas, 1999

机译：人黑素瘤细胞系和异种移植物中的基质金属蛋白酶：激活的基质金属蛋白酶2（MMP-2）的表达增加与黑色素瘤的进展有关
7. Increased cellular expression of matrix proteins that regulate mineralization is associated with calcification of native human and porcine xenograft bioprosthetic heart valves. [O] . Srivatsa, S S, Harrity, P J, Maercklein, P B, 1997

机译：调节矿化作用的基质蛋白的细胞表达增加与天然人和猪异种移植生物瓣膜的钙化有关。

Increased cellular expression of matrix proteins that regulate mineralization is associated with calcification of native human and porcine xenograft bioprosthetic heart valves.

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