Towards a Novel Treatment Strategy for Acute Pancreatitis

Abstract: Despite more than a century of research endeavour, there is no specific medical treatment for acute pancreatitis and early mortality is high – 20% of fatalities by the day after admission. I do not see any realistic prospect that today’s focus on immunomodulation will provide a breakthrough either. The signs are that the outcome of acute pancreatitis is determined almost at its inception, and that those unfortunate individuals in whom the seeds for a precipitous course are sewn do not declare themselves until … Show more

“…2 The evolution of an attack of severe pancreatitis precipitated by percutaneous pancreatic biopsy two days after ERCP – with particular reference to blood antioxidant consumption in the first few days, despite prior antioxidant supplementation. As discussed in the text and in earlier reports [1, 2], the abrupt consumption of plasma ascorbate/vitamin C is best explained by histamine oxidation products: an anaphylactoid response of pancreatic mast cells may have been precipitated by pethidine and/or lignocaine. The patient is a man aged 41 years, fit until six months before presentation with incapacitating epigastric pain following two attacks, and computed tomography evidence of calcific chronic pancreatitis with a mass in the head of the gland.…”

“…As was observed in part 1 [1], the high early mortality of acute pancreatitis – 20% of deaths by the day after admission and 40% by the next day – is best rationalised in terms of mast cell pathology. Figure 1 illustrates how the concept links with the disease-initiating burst of free radical activity which paralyses the secretory pathway towards exocytosis in the acinar cell.…”

“…ZG = zymogen granules; L = lysosomes; V = vacuoles in cytoplasm; ROS = reactive oxygen species; RXS = reactive xenobiotic species generated via pancreatic cytochrome P450, alcohol/acetaldehyde dehydrogenases or prostaglandin synthase; N = nucleus; FROPs = free radical oxidation products; PAF = platelet activating factor; NO · = nitric oxide; LTB 4 and LTC 4 = leukotrienes; PGD 2 = prostaglandin D 2 ; IFN-α = interferon-α; IL-1,6,8 = interleukin series; TNF-α = tumour necrosis factor-α; EC = endothelial cell; PMN = neutrophil; P = platelet; MΦ = macrophage; PLA 2 = cell membrane-lysing form of phospholipase A 2 which could hydrolyse adipocyte membranes to facilitate lipase entry, and thus fat necrosis; tPA, uPA = tissue-type and urokinase plasminogen activator, respectively; PAR-2 proteinase activated receptor-2; C3 = complement subtype; ⊕ = activation; AO = antioxidants; LA-OP = linoleic acid oxidation products. Note that a high degree of oxidative stress (represented by the scales at the bottom) and the participation of reactive xenobiotic species – including those derived from linoleic acid and opiate analgesics [1, 2] – favours an anaphylactoid reaction of mast cells. …”

“…Schematic representation of the ‘free radical-mast cell’ template for the aetiogenesis of acute pancreatitis based on published information [1, 2]. The large cross symbol at the apical pole of the acinar cell indicates the disease-initiating blockade to exocytosis, which leads to a reversal in secretory polarity such that pro-inflammatory substances enter the interstitium along with the cell’s normal secretions.…”

“…Further, for this enzyme the increase seems to be selective for the development of acute pancreatitis – unusual when hyperamylasemia is asymptomatic – and its increment higher in severe than mild disease [16]. However, a clear increase in anionic trypsin-α 1 proteinase inhibitor complexes within serum is not seen until 24 h, when levels in severe pancreatitis are of the same order as in mild disease [16]: moreover it can be calculated that the active enzyme constitutes <10% of the circulating zymogen load [1]. This delay explains the lack of increase in the urinary concentration of the trypsinogen activation peptide (TAP) when sought at 4 h [17], but an increase at 24 h of the carboxypeptidase B activation peptide (CAPAP) [18], surrogate marker of trypsinogen activation [19].…”

Towards a Novel Treatment Strategy for Acute Pancreatitis

“…2 The evolution of an attack of severe pancreatitis precipitated by percutaneous pancreatic biopsy two days after ERCP – with particular reference to blood antioxidant consumption in the first few days, despite prior antioxidant supplementation. As discussed in the text and in earlier reports [1, 2], the abrupt consumption of plasma ascorbate/vitamin C is best explained by histamine oxidation products: an anaphylactoid response of pancreatic mast cells may have been precipitated by pethidine and/or lignocaine. The patient is a man aged 41 years, fit until six months before presentation with incapacitating epigastric pain following two attacks, and computed tomography evidence of calcific chronic pancreatitis with a mass in the head of the gland.…”

“…As was observed in part 1 [1], the high early mortality of acute pancreatitis – 20% of deaths by the day after admission and 40% by the next day – is best rationalised in terms of mast cell pathology. Figure 1 illustrates how the concept links with the disease-initiating burst of free radical activity which paralyses the secretory pathway towards exocytosis in the acinar cell.…”

“…ZG = zymogen granules; L = lysosomes; V = vacuoles in cytoplasm; ROS = reactive oxygen species; RXS = reactive xenobiotic species generated via pancreatic cytochrome P450, alcohol/acetaldehyde dehydrogenases or prostaglandin synthase; N = nucleus; FROPs = free radical oxidation products; PAF = platelet activating factor; NO · = nitric oxide; LTB 4 and LTC 4 = leukotrienes; PGD 2 = prostaglandin D 2 ; IFN-α = interferon-α; IL-1,6,8 = interleukin series; TNF-α = tumour necrosis factor-α; EC = endothelial cell; PMN = neutrophil; P = platelet; MΦ = macrophage; PLA 2 = cell membrane-lysing form of phospholipase A 2 which could hydrolyse adipocyte membranes to facilitate lipase entry, and thus fat necrosis; tPA, uPA = tissue-type and urokinase plasminogen activator, respectively; PAR-2 proteinase activated receptor-2; C3 = complement subtype; ⊕ = activation; AO = antioxidants; LA-OP = linoleic acid oxidation products. Note that a high degree of oxidative stress (represented by the scales at the bottom) and the participation of reactive xenobiotic species – including those derived from linoleic acid and opiate analgesics [1, 2] – favours an anaphylactoid reaction of mast cells. …”

“…Schematic representation of the ‘free radical-mast cell’ template for the aetiogenesis of acute pancreatitis based on published information [1, 2]. The large cross symbol at the apical pole of the acinar cell indicates the disease-initiating blockade to exocytosis, which leads to a reversal in secretory polarity such that pro-inflammatory substances enter the interstitium along with the cell’s normal secretions.…”

“…Further, for this enzyme the increase seems to be selective for the development of acute pancreatitis – unusual when hyperamylasemia is asymptomatic – and its increment higher in severe than mild disease [16]. However, a clear increase in anionic trypsin-α 1 proteinase inhibitor complexes within serum is not seen until 24 h, when levels in severe pancreatitis are of the same order as in mild disease [16]: moreover it can be calculated that the active enzyme constitutes <10% of the circulating zymogen load [1]. This delay explains the lack of increase in the urinary concentration of the trypsinogen activation peptide (TAP) when sought at 4 h [17], but an increase at 24 h of the carboxypeptidase B activation peptide (CAPAP) [18], surrogate marker of trypsinogen activation [19].…”

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