CASE 15441 Published on 27.01.2018
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Hypertriglyceridaemia-related recurrent acute pancreatitis with splenic vein thrombosis

Section

Abdominal imaging

Case Type

Clinical Cases

Authors

Tonolini Massimo, MD.

"Luigi Sacco" University Hospital,Radiology Department; Via G.B. Grassi 74 20157 Milan, Italy; Email:mtonolini@sirm.org
Connected authors
Patient

41 years, male

Categories
Area of Interest Pancreas ; Imaging Technique MR, Ultrasound, CT, Ultrasound-Colour Doppler
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Clinical History
Overweight young adult male patient presenting to emergency department with upper abdominal pain, without peritonism at physical examination. History included heavy cigarette smoking, gastritis, chronic hepatitis C infection.
Routine laboratory tests showed mild leukocytosis, elevated liver transaminases (AST 240 - ALT 120 U/l), amylase (330 U/l), gamma-glutamytranspeptidase (367 U/l); normal bilirubin.
Imaging Findings
Ultrasound (Fig.1) showed liver steatosis, normal-sized pancreas, normal gallbladder and bile ducts. The next day, CT (Fig.2) requested to investigate clinical diagnosis of acute pancreatitis (AP) showed left-sided peripancreatic and fascial effusion, normal pancreas with focal hypoenhancement at the tail consistent with <30% necrosis, and partial splenic vein thrombosis. The patient had stopped drinking alcohol years earlier, and marked increase of serum triglycerides (2515 mg/dl) underlying AP was noted.
Supportive treatment plus low-molecular-weight heparin allowed clinical resolution. Follow-up colour-Doppler ultrasound (Fig.3) after discharge showed disappearance of thrombosis.
Nine months later (after having stopped fibrate therapy) the patient experienced recurrent AP with left-sided abdominal pain, elevated amylase and lipase levels, and severely increased triglycerides (9700 mg/dl). At MRI (Figs.4, 5) a post-necrotic collection had developed at the pancreatic tail, segmental oedematous AP appeared as restricted diffusion at pancreatic head and neck, without peripancreatic fluid, gallbladder and ductal abnormalities at MR-cholangiopancreatography (Fig.4e).
Discussion
Albeit rare, severe hypertriglyceridaemia (HTG) is well-established aetiology of acute pancreatitis (AP). HTG over 1000 mg/dL is present in 1.7% of the adult population, it may trigger AP development in 5.4-20% of affected patients, and accounts for 2-10% of all AP occurrences thus representing the third leading cause after gallstones and alcohol. The pathophysiology of HTG-induced AP involves hydrolysis of triglycerides by pancreatic enzymes, hyperviscosity and ischaemia, excessive formation of free fatty acids and lysolecithin from the lipoprotein substrates in the pancreatic bed, leading to overload of the albumin capacity, damage of acinar cells and microvascular (capillary) membranes [1-5].
In some patients, HTG is familiar or secondary to inborn errors of metabolism. Most usually, HTG is encountered in patients with multiple comorbidities such as obesity, diabetes, history of alcohol abuse, renal disease and multiple medications. In these patients, HTG is underdiagnosed and undertreated, in part because of poor compliance to lipid-lowering therapy. For each 100 mg/dl unit of increase in the triglycerides level above 1000 mg/dL, there is a 3% increase of AP risk. The majority of patients suffering from HTG-related AP are young adults (median±standard deviation 39-45±8-10 years) with a 57-70% male predominance. Clinical manifestations and supportive treatment are analogous to those of AP from other causes, but there is consensus that HTG-related AP is often a severe form with high rates of intensive care unit admission (32%). In these patients, amylase levels may be falsely low due to milk-consistency serum. Cross-sectional imaging shows a high prevalence of parenchymal (31%) and peripancreatic (14%) necrosis. As a result, development of acute post-necrotic collections and walled-off pancreatic necrosis is very common (44% of patients) compared to the rarity of pseudocysts. Chronic pancreatitis is reported in 16% of patients [1, 3-7].
As in this patient, further complications such as venous thrombosis may develop, probably resulting from the well-known AP-associated hypercoagulability state including higher plasma levels of fibrinogen and factor VIII, which require anticoagulation [8].
In the acute phase, treatment aims at rapidly decreasing serum triglycerides levels, includes intravenous insulin and may benefit from plasmapheresis. Lifestyle modifications and lipid-lowering drugs (fibrates alone or in conjunction with statins) allow reducing the risk of recurrence [1, 2, 7].
Differential Diagnosis List
Hypertriglyceridaemia-related recurrent acute necrotising pancreatitis with splenic vein thrombosis
Oedematous acute pancreatitis
Gallstone-related acute pancreatitis
Alcohol-related acute pancreatitis
Drug-induced acute pancreatitis
Hypercoagulable condition
Final Diagnosis
Hypertriglyceridaemia-related recurrent acute necrotising pancreatitis with splenic vein thrombosis
Case information
URL: https://eurorad.org/case/15441
DOI: 10.1594/EURORAD/CASE.15441
ISSN: 1563-4086
License

This work is licensed under a Creative Commons Attribution-NonCommercial-ShareAlike 4.0 International License.

Figure 1

Bedside abdominal ultrasound at emergency admission

Bedside abdominal ultrasound at emergency admission
Sonography revealed hepatomegaly with markedly hyperechoic echotexture consistent with severe steatosis; normal gallbladder without lithiasis and inflammation; absent biliary dilatation.
Bedside abdominal ultrasound at emergency admission
The visible pancreatic portions (+) did not appear enlarged. Peripancreatic effusion and fluid collections were not seen.
Figure 2

Unenhanced and post-contrast multidetector CT (24 hours after Fig.1)

Unenhanced and post-contrast multidetector CT (24 hours after Fig.1)
Precontrast images (a,b) showed effusion (*) surrounding the spleen and pancreatic tail, extending to the left retroperitoneal fasciae. Note hypoattenuating parenchyma consistent with marked liver steatosis.
Unenhanced and post-contrast multidetector CT (24 hours after Fig.1)
Precontrast images (a,b) showed effusion (*) surrounding the spleen and pancreatic tail, extending to the left retroperitoneal fasciae. The pancreas (+) did not appear enlarged. Note hypoattenuating parenchyma consistent with marked liver steatosis.
Unenhanced and post-contrast multidetector CT (24 hours after Fig.1)
After iv contrast, the normal-sized pancreas showed focal hypoenhancement at the tail (arrowheads) consistent with necrosis (<30%). Note peripancreatic and fascial fluid (*), marked liver steatosis, normal gallbladder.
Unenhanced and post-contrast multidetector CT (24 hours after Fig.1)
After iv contrast, the normal-sized pancreas showed focal hypoenhancement at the tail (arrowheads) consistent with necrosis (<30%). Note peripancreatic and fascial fluid (*), marked liver steatosis.
Unenhanced and post-contrast multidetector CT (24 hours after Fig.1)
Additionally, filling defect (thin arrows) indicating partial thrombosis of the splenic vein was noted. Note peripancreatic and fascial fluid (*), patent portal and mesenteric veins, marked liver steatosis.
Unenhanced and post-contrast multidetector CT (24 hours after Fig.1)
After iv contrast, the normal-sized pancreas showed focal hypoenhancement at the tail (arrowheads) consistent with necrosis (<30%). Note peripancreatic and fascial fluid (*), marked liver steatosis.
Unenhanced and post-contrast multidetector CT (24 hours after Fig.1)
Additionally, filling defect (thin arrows) indicating partial thrombosis of the splenic vein was noted. Note peripancreatic and fascial fluid (*), patent portal and mesenteric veins, marked liver steatosis.
Figure 3

Colour Doppler ultrasound (CDUS) 6 weeks later

Colour Doppler ultrasound (CDUS) 6 weeks later
CDUS follow-up showed patent splenic vein with normal flow spectrum (a) and direction (b) consistent with resolution of thrombosis.
Colour Doppler ultrasound (CDUS) 6 weeks later
CDUS follow-up showed patent splenic vein with normal flow spectrum (a) and direction (b) consistent with resolution of thrombosis.
Colour Doppler ultrasound (CDUS) 6 weeks later
Normal flow direction and spectrum in the portal vein.
Figure 4

MRI (9 months later) - T2- and diffusion-weighted images

MRI (9 months later) - T2- and diffusion-weighted images
At clinical relapse, the pancreas maintained normal size. A demarcated post-necrotic collection (arrowheads) had developed at the tail, corresponding to site of initial necrosis (Fig.2), with low T2-weighted signal reflecting fibrosis.
MRI (9 months later) - T2- and diffusion-weighted images
At clinical relapse, the pancreas maintained normal size. A demarcated post-necrotic collection (arrowheads) had developed at the tail, corresponding to site of initial necrosis (Fig.2), with low T2-weighted signal reflecting fibrosis.
MRI (9 months later) - T2- and diffusion-weighted images
At clinical relapse, the pancreas maintained normal size. A demarcated post-necrotic collection (arrowheads) had developed at the tail, corresponding to site of initial necrosis (Fig.2), with low T2-weighted signal reflecting fibrosis.
MRI (9 months later) - T2- and diffusion-weighted images
At clinical relapse, the pancreas maintained normal size, without peripancreatic fluid on fat-suppressed T2-weighted acquisition. Note non-dilated main bile duct, normal-appearing gallbladder.
MRI (9 months later) - T2- and diffusion-weighted images
MR-cholangiopancreatography confirmed normal-appearing gallbladder, intrahepatic and common bile ducts. The Wirsung duct did not show appreciable abnormalities.
MRI (9 months later) - T2- and diffusion-weighted images
High (800) b-value diffusion-weighted images (f,g) showed increased signal in the pancreatic (+) head and neck compared to body-tail, with corresponding low apparent diffusion coefficient (h,i) indicating segmental acute inflammation.
MRI (9 months later) - T2- and diffusion-weighted images
High (800) b-value diffusion-weighted images (f,g) showed increased signal in the pancreatic (+) head and neck compared to body-tail, with corresponding low apparent diffusion coefficient (h,i) indicating segmental acute inflammation.
MRI (9 months later) - T2- and diffusion-weighted images
High (800) b-value diffusion-weighted images (f,g) showed increased signal in the pancreatic (+) head and neck compared to body-tail, with corresponding low apparent diffusion coefficient (h,i) indicating segmental acute inflammation.
MRI (9 months later) - T2- and diffusion-weighted images
The post-necrotic collection (arrowheads) did not show restricted diffusion (ADC map i, b800 image j).
Figure 5

MRI (9 months later) - T1-weighted images w/o gadolinium

MRI (9 months later) - T1-weighted images w/o gadolinium
On precontrast fat-suppressed T1-weighted images, the post-necrotic collection (arrowhead) at the pancreatic tail showed inhomogeneous, intermediate signal intensity consistent with partly fibrotic component.
MRI (9 months later) - T1-weighted images w/o gadolinium
Dynamic gadolinium-enhanced acquisition (b...e) showed normally enhancing pancreatic gland (detail of head an neck in b, body, in c, tail in d), absent enhancement of the distal post-necrotic collection (arrowheads in d-e).
MRI (9 months later) - T1-weighted images w/o gadolinium
Dynamic gadolinium-enhanced acquisition (b...e) showed normally enhancing pancreatic gland (detail of head an neck in b, body, in c, tail in d), absent enhancement of the distal post-necrotic collection (arrowheads in d-e).
MRI (9 months later) - T1-weighted images w/o gadolinium
Dynamic gadolinium-enhanced acquisition (b...e) showed normally enhancing pancreatic gland (detail of head an neck in b, body, in c, tail in d), absent enhancement of the distal post-necrotic collection (arrowheads in d-e).
MRI (9 months later) - T1-weighted images w/o gadolinium
Dynamic gadolinium-enhanced acquisition (b...e) showed normally enhancing pancreatic gland (detail of head an neck in b, body, in c, tail in d), absent enhancement of the distal post-necrotic collection (arrowheads in d-e).