Quantitative Estimation of the Collagen Content in Normal and Pathologic Pancreas Tissue

Bedossa, P.; Lemaigre, G; Bacci, Josette; Martin, E

doi:10.1159/000199886

Cited by 42 publications

(21 citation statements)

References 12 publications

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“…Total pancreatic collagen in established chronic pancreatitis may be some three times higher than normal [26]. The types of collagen deposited have been characterized as types I and III within regions of interlobular fibrosis but type III only within regions of intralobular fibrosis [14], In the present study, more wide spread TGF-Pi expression was identified in the ductules in chronic pancreatitis than in normal pancreatic tissues.…”

Section: Discussionmentioning

confidence: 45%

Expression of Transforming Growth Factor-β<sub>1</sub> in Chronic Pancreatitis

Slater¹,

Williamson

Foster

1995

Digestion

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Transforming growth factor-β₁ (TGF-β₁) is a multifunctional cytokine which modifies tissue stromal matrix synthesis, cell proliferation and immune function. In the present study, we have used a mouse monoclonal antibody to the latent (intracytoplasmic) form of TGF-β₁ to compare its expression in 144 cases of human chronic pancreatitis (both obstructive and chronic calcifying) with that of 10 control pancreatic specimens. In all the control specimens, and most of those with chronic pancreatitis, cytoplasmic immunoreactivity was identified in pancreatic duct and ductular epithelium, in islet cells and in vascular smooth muscle and endothelium. Two distinct patterns of ductular epithelial staining emerged: in morphologically normal tissues, only individual distal ductular/centroacinar cells stained but in chronic pancreatitis (whether chronic calcifying or chronic obstructive) the staining was panductular. Positive cytoplasmic immunostaining of acinar epithelial cells was found in 3% of pancreatitis specimens but in none of the normal controls. There was no staining of fibroblasts. Synthesis of TGF-β₁ appears to be normally restricted to a population of epithelial cells located in terminal/centroacinar regions of the ductules (together with occasional ductal cells) whereas in chronic pancreatitis, TGF-β₁ is expressed in most ductular and ductal epithelial cells.

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Section: Discussionmentioning

confidence: 45%

Expression of Transforming Growth Factor-β<sub>1</sub> in Chronic Pancreatitis

Slater¹,

Williamson

Foster

1995

Digestion

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“…an even more rapid accumulation of periacinar fibrosis and altered acinar architecture and resulted in a pattern of fibrosis similar to that found in human chronic pancreatitis (Bedossa et al, 1989;Pitchumoni et al, 1984;Suda et al, 1990). The observation that the pancreatic fibrosis began to resolve after injury was stopped suggests that the processes responsible for matrix resolution are potently active in the pancreas.…”

Section: Neuschwander-tetri Et Almentioning

confidence: 65%

“…The affinity of the sirius red chromophore via its sulphonic acid group for the amino acid composition of collagen confers excellent selectivity of this dye for collagen and has been used previously to quantify tissue collagen by both spectrophotometric and image analysis methods (Chevallier et al, 1994;Pilette et al, 1998). In normal human pancreas, sirius red staining demonstrates collagen around ducts and within the interlobular septae (Bedossa et al, 1989). As shown in Figure 2, collagen deposition increased during 6 weeks of treatment and diminished but did not normalize during an equal period of recovery.…”

Section: Resultsmentioning

confidence: 99%

Repetitive Acute Pancreatic Injury in the Mouse Induces Procollagen α1(I) Expression Colocalized to Pancreatic Stellate Cells

Neuschwander‐Tetri¹,

Bridle

Wells³

et al. 2000

Laboratory Investigation

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SUMMARY:Pancreatic stellate cells may be a major source of extracellular matrix deposition during injury. This study was undertaken to establish whether pancreatic stellate cells are a source of Type I collagen in vivo and whether they continue to be a source of matrix production in the post-injury fibrotic pancreas. To induce pancreatic fibrogenesis, acute pancreatic injury was induced in mice three times weekly with supraphysiologic doses of cerulein. Animals were treated for 6 weeks and allowed to recover for an additional 6 weeks. Stellate cell activation and pancreatic collagen expression were measured by immunohistochemistry, whole tissue RNA analysis, and in situ hybridization. Histology and digital image analysis demonstrated the development of substantial pancreatic fibrosis after 6 weeks of treatment. During recovery, incomplete resolution of the fibrosis was found. Procollagen ␣ 1 (I) mRNA increased more than15-fold during treatment and continued to be 5-fold elevated during the post-injury phase. In situ hybridization studies demonstrated that collagen gene expression was colocalized to activated pancreatic stellate cells. Collagen expression and fibrosis persisted in focal areas during recovery. These findings show that pancreatic stellate cells are the major source of collagen during repetitive injury in vivo. Additionally, focal areas of sustained pancreatic fibrogenesis persist after cessation of cerulein treatment, and these areas may contribute to sustained total organ collagen expression in the absence of ongoing injury. (Lab Invest 2000, 80:143-150).

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“…In humans it has been shown that increasing amount of collagen makes islet isolation less successful (Bedossa et al, 1989). However, we did not attempt to quantify peri-islet matrix in order to clarify the effect of collagen on the efficiency of islet isolation.…”

Section: Insulin Mrna Quantities In Isolated Isletsmentioning

confidence: 99%