Abstract
Several pancreatitis susceptibility genes have been identified to date. A relationship between a mutation in the cationic trypsinogen (protease serine 1, PRSS1) gene and hereditary pancreatitis (HP) was first identified in 1996. Currently, HP has been defined as either two or more individuals within a family exhibiting pancreatitis for two or more generations, or pancreatitis linked to mutation of the PRSS1 gene. In 2000, a mutation in the serine protease inhibitor gene (Kazal type 1: SPINK1) was reported to be related to sporadic pancreatitis of unknown etiology. This paper reviews and summarizes the current published data on the pancreatitis susceptibility genes, mainly PRSS1 and SPINK1 genes, and introduces a diagnostic and therapeutic approach for dealing with patients with these gene mutations. Patients with these genetic predispositions, both children and adults, have often been initially diagnosed with idiopathic acute pancreatitis, in approximately 20–50% of pediatric cases and 28–80% of adult cases. In such patients, where the etiology is unknown, genetic testing, which requires pre-test and post-test genetic counselling, may prove helpful. Patients with chronic pancreatitis (CP) due to SPINK1 gene mutation and HP patients have a potentially high risk of pancreatic exocrine insufficiency, diabetes mellitus, and, of particular importance, pancreatic cancer. Thus, these patients require careful long-term follow-up and management. Specifically, symptomatic CP patients often need endoscopic therapy or surgery, often following a step-up approach beginning with endoscopic therapy and progressing to surgery if necessary, which is similar to the therapeutic approach for patients with CP due to other etiologies. It is important that clinicians are aware of the characteristics of patients with pancreatitis susceptibility genetic abnormalities.
Highlights
When the patients with acute recurrent pancreatitis (ARP) or chronic pancreatitis (CP) showing autosomal dominant pattern of inheritance, these demographics have been characterized hereditary pancreatitis (HP)
As damage to the pancreas progresses, malabsorption occurs due to pancreatic exocrine insufficiency, and diabetes mellitus develops due to pancreatic islet cell damage [3]
According to the European Registry of Hereditary Pancreatitis and Familial Pancreatic Cancer (EUROPAC), a diagnosis of HP can be made without genetic testing if the patient has both a personal history of pancreatitis and APR, or has CP been diagnosed in two first-degree relatives or in three or more second-degree relatives, spanning at least two generations [37]
Summary
When the patients with acute recurrent pancreatitis (ARP) or chronic pancreatitis (CP) showing autosomal dominant pattern of inheritance, these demographics have been characterized hereditary pancreatitis (HP). HP caused by cationic trypsinogen (serine protease 1; PRSS1) gene mutation results in ARP and CP in both children and adults with high penetrance [1,2]. As damage to the pancreas progresses, malabsorption occurs due to pancreatic exocrine insufficiency, and diabetes mellitus develops due to pancreatic islet cell damage [3]. Several cohorts showed the natural history of patients with serine protease inhibitor gene (Kazal type 1: SPINK1) germline-related pancreatitis and HP caused by PRSS1 gene mutation, indicating a high progression rate of pancreatic exocrine insufficiency and diabetes mellitus, as well as a significantly increased risk of pancreatic cancer [3,7]. This paper reviews and summarizes the currently published data on the genetic abnormalities of pancreatitis susceptibility genes, and introduces a diagnostic and therapeutic approach for patients with these gene mutations
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