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FACULTYOPINIONS . COM {}

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We began analyzing https://archive.connect.h1.co/article/1025421/, but it redirected us to https://archive.connect.h1.co/article/1025421/. The analysis below is for the second page.

Title[redir]:
Properties of the permeability tra ... | Article | H1 Connect
Description:
We have studied the properties of the permeability transition pore (PTP) in mitochondria from the liver of mice where the Ppif gene encoding for mitochondr

Matching Content Categories {πŸ“š}

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  • Education

Content Management System {πŸ“}

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Custom-built

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Traffic Estimate {πŸ“ˆ}

What is the average monthly size of facultyopinions.com audience?

πŸš— Small Traffic: 1k - 5k visitors per month


Based on our best estimate, this website will receive around 4,276 visitors per month in the current month.

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Keywords {πŸ”}

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Topics {βœ’οΈ}

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Questions {❓}

  • Regulated and unregulated mitochondrial permeability transition pores: a new paradigm of pore structure and function?

Schema {πŸ—ΊοΈ}

ScholarlyArticle:
      context:https://schema.org
      headline:Properties of the permeability transition pore in mitochondria devoid of Cyclophilin D.
      abstract:We have studied the properties of the permeability transition pore (PTP) in mitochondria from the liver of mice where the Ppif gene encoding for mitochondrial Cyclophilin D (CyP-D) had been inactivated. Mitochondria from Ppif-/- mice had no CyP-D and displayed a striking desensitization of the PTP to Ca2+, in that pore opening required about twice the Ca2+ load necessary to open the pore in strain-matched, wild-type mitochondria. Mitochondria lacking CyP-D were insensitive to Cyclosporin A (CsA), which increased the Ca2+ retention capacity only in mitochondria from wild-type mice. The PTP response to ubiquinone 0, depolarization, pH, adenine nucleotides, and thiol oxidants was similar in mitochondria from wild-type and Ppif-/- mice. These experiments demonstrate that (i) the PTP can form and open in the absence of CyP-D, (ii) that CyP-D represents the target for PTP inhibition by CsA, and (iii) that CyP-D modulates the sensitivity of the PTP to Ca2+ but not its regulation by the proton electrochemical gradient, adenine nucleotides, and oxidative stress. These results have major implications for our current understanding of the PTP and its modulation in vitro and in vivo.
      hasPart:
         type:WebPageElement
         isAccessibleForFree:
         cssSelector:.paywalled-content
      isAccessibleForFree:
      mainEntityOfPage:
         type:WebPage
         id:https://connect.h1.co/article/1025421
WebPage:
      id:https://connect.h1.co/article/1025421

External Links {πŸ”—}(40)

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