Guest guest Posted March 13, 2009 Report Share Posted March 13, 2009 Dear Stevie; Regarding your question about whether or not liver fibrosis is reversible (repairable), I'd like to comment that it can be reversed/repaired in animal models, but research still needs to be done to extend this to human subjects. One of the big factors causing liver fibrosis seems to be that the main vitamin A-storing cells in the liver, hepatic stellate cells, lose all of their vitamin A (retinol) during inflammation. This loss of vitamin A then triggers the hepatic stellate cells to produce collagen. The key to fibrosis seems to be the balance between collagen synthesis rate versus collagen degradation rate. If collagen synthesis exceeds collagen degradation then liver fibrosis advances. But if collagen synthesis can be blocked, while continued collagen degradation is allowed to occur, then reversal of fibrosis can ensue. In this paper they show that in experimental animal models of liver fibrosis, if an inhibitor of collagen synthesis is wrapped in a vitamin-A coated liposome (tricking the hepatic stellate cells into taking up the inhibitor), this blocks collagen synthesis, essentially preventing (and reversing) liver fibrosis: ____________________________ Nat Biotechnol. 2008 Apr;26(4):431-42. Resolution of liver cirrhosis using vitamin A-coupled liposomes to deliver siRNA against a collagen-specific chaperone. Sato Y, Murase K, Kato J, Kobune M, Sato T, Kawano Y, Takimoto R, Takada K, Miyanishi K, Matsunaga T, Takayama T, Niitsu Y. Fourth Department of Internal Medicine, Sapporo Medical University, School of Medicine, Sapporo, 060-8543, Japan. There are currently no approved antifibrotic therapies for liver cirrhosis. We used vitamin A-coupled liposomes to deliver small interfering RNA (siRNA) against gp46, the rat homolog of human heat shock protein 47, to hepatic stellate cells. Our approach exploits the key roles of these cells in both fibrogenesis as well as uptake and storage of vitamin A. Five treatments with the siRNA-bearing vitamin A-coupled liposomes almost completely resolved liver fibrosis and prolonged survival in rats with otherwise lethal dimethylnitrosamine-induced liver cirrhosis in a dose- and duration-dependent manner. Rescue was not related to off-target effects or associated with recruitment of innate immunity. Receptor-specific siRNA delivery was similarly effective in suppressing collagen secretion and treating fibrosis induced by CCl(4) or bile duct ligation. The efficacy of the approach using both acute and chronic models of liver fibrosis suggests its therapeutic potential for reversing human liver cirrhosis. PMID: 18376398. ________________________ This is one of the many reasons why I am interested in vitamin A (retinol) and its derivative (retinoic acid) in the progression of PSC. Best regards, Dave (father of (23); PSC 07/03; UC 08/03) > From what I understand fibrosis is not repairable, does anyone know if that is Fact?? Quote Link to comment Share on other sites More sharing options...
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