Bo Yu, Rana Douli, Jose Amaya Suarez, Victor Perez Gutierrez, Mohammad Aldiabat, Maria Khan

Bo Yu, Rana Douli, Jose Amaya Suarez, Victor Perez Gutierrez, Mohammad Aldiabat, Maria Khan, Department of Medicine, Lincoln Medical Center, Bronx, NY 10451-5504, United States

Abstract

Key words: Non-islet cell tumor hypoglycemia; Hepatocellular carcinoma; Liver cirrhosis; Insulin-like growth factor-2; Paraneoplastic syndrome; Case report

INTRODUCTION

Non-islet cell tumor hypoglycemia (NICTH) is a rare paraneoplastic complication associated with malignancies of both epithelial and mesenchymal origin. One of the most common epithelial tumors is hepatocellular carcinoma (HCC)[1,2]. Hypoglycemia is induced either by tumor consumption of glucose (type A) or overproduction of incompletely processed insulin-like growth factor-2 (IGF-2) (type B), while levels of insulin, C-peptide, pro-insulin, and beta-hydroxybutyrate are suppressed[3]. NICTH occurs in 4% to 27% of patients with HCC[4]. However the actual prevalence might be underestimated due to limited availability of testing for IGF-2. In addition, the etiologies of hypoglycemia in HCC patients are often multifactorial. Many patients might have developed tolerance to chronic fasting hypoglycemia due to long term poor hepatic function and nutritional status at the time of discovery of HCC. Here we report a case of persistent NICTH as the initial presentation in a patient with newly diagnosed HCC overlapped with end-stage liver cirrhosis.

CASE PRESENTATION

Chief complaints

A 62-year-old Hispanic male with long-standing hepatitis C-related cirrhosis was brought to the emergency room on December 7, 2019 due to 2 episodes of altered mental status and non-vertiginous dizziness witnessed by his family. He also reported an unintentional 1-kg weight loss over the past 1 mo.

History of present illness

There was no history of loss of consciousness, falls, or head trauma. He was first found to have hepatitis C infection with concurrent liver cirrhosis and portal hypertension in 2015. Viral load became undetectable after the completion of antiviral therapy but the patient lost follow-up ever since July 2018. Child-Pugh score during the last outpatient visit was 8 (class B). AFP was within the normal limit. No signs of malignancy were found on liver ultrasound.

Physical examination upon admission

On physical exam, he was all the time conscious and had full ability to communicate. Vital signs were within normal limits. Rest of the physical exam was significant for cachectic appearance, jaundice, and bilateral lower extremity edema up to the knee.

Laboratory examination, imaging studies and diagnostic reasoning

In the emergency room, his blood glucose was detected to be 26 mg/dL. He denied poor oral intake or history of diabetes, alcohol abuse or illicit drug use. Of note, his blood glucose level tended to be on the lower side (75-85 mg/dL) seen in the records of several outpatient visits before he lost follow-up. The blood glucose level was corrected by two immediate intravenous 50% dextrose pushes, but dropped again down to 10 mg/dL in 2 h for which continuous 10% dextrose infusion was started and the patient was instructed to consume frequent carbohydrate-rich snacks. However, recurrent hypoglycemic attacks still occurred since admission that required multiple IV 50% dextrose and glucagon pushes.

Laboratory evaluation of hypoglycemia showed undetectable insulin [< 0.4 µU/mL (2.6-24.9 µU/mL)], low C-peptide [0.2 ng/mL (1.1-4.4 ng/mL)], lower normal proinsulin [1.3 pmol/L (0-10.0 pmol/L)], and undetectable beta-hydroxybutyrate [< 0.1 mg/dL (0.2-2.8 mg/dL)], excluding the possibility of insulinoma. Sulfonylurea screen test was negative. Adrenal insufficiency was also unlikely due to a high serum cortisol concentration. His hepatic function deteriorated [INR 2.8; albumin 2.9 g/dL (3.5-5.2 g/dL); total bilirubin 3.76 mg/dL (0.2-1.2 mg/dL); aspartate transaminase 145 U/L (< 40 U/L); alanine transaminase 93 U/L (< 41 U/L); alkaline phosphatase 263 U/L (40-130 U/L)]. Hepatic encephalopathy was also suspected due to high ammonia level [101 µmol/L (16-60 µmol/L)]. Child-Pugh score was calculated to be 11 (class C). AFP level was found to be elevated [108 ng/mL (< 8.3 ng/mL)]. Computed tomography of the abdomen with contrast showed cirrhosis and there was a centrally necrotic mass in the left hepatic lobe, measuring 6.7 cm × 6.5 cm (Figure 1). Three-phase liver computed tomography scan demonstrated suboptimal arterial phase enhancement due to the timing of the contrast with washout on delayed phase of the study. A subsequent biopsy confirmed the diagnosis of well differentiated HCC. No metastasis was found on bone scan. Therefore, NICTH was suspected. To establish the diagnosis, serum insulin-like growth factor-1 (IGF-1), IGF-2, and insulin-like growth factor-binding protein 3, the major binding protein for IGF-2 were measured. IGF-1 was suppressed [14 ng/mL (49-214 ng/mL)], IGF-2 was lower normal [303 ng/mL (300-960 ng/mL)], insulin-like growth factor-binding protein 3 was slightly decreased [2.2 µg/mL (2.6-4.8 µg/mL)], and the IGF-2/IGF-1 ratio was 21.6 (> 10), consistent with the diagnosis of NICTH.

FINAL DIAGNOSIS

NICTH (type B); well differentiated HCC, Barcelona Clinic Liver Cancer Stage D; decompensated liver cirrhosis, Child-Pugh Class C.

TREATMENT

The patient was not a candidate of transplant, surgical resection, or palliative chemotherapy due to the baseline poor hepatic function. He was started on oral prednisolone with a dose titrated up to 60 mg daily. There were less hypoglycemic episodes and the patient showed improvements in the severity of hypoglycemia. However, he still required on and off glucose supplements to maintain glucose homeostasis. While waiting for the trial of trans-arterial chemoembolization and radiotherapy, he developed hospital-acquired pneumonia. And concurrently his plasma glucose dropped and became difficult to correct again (Figure 2).

OUTCOME AND FOLLOW-UP

The patient opted for inpatient hospice care and died of septic shock on day 19 of hospitalization.

DISCUSSION

NICTH is a rare complication seen in patients with HCC. In the present case, the patient had advanced cirrhosis without regular follow up for a year, so it’s unclear when the HCC first developed. Interestingly, acute hypoglycemic encephalopathy occurred as the sole initial clinical symptom prior to the diagnosis of HCC. Different from a few previously reported cases[5-9], our patient had a very poor hepatic function and nutritional status which could both contribute to his hypoglycemia to some extent. He might have developed chronic hypoglycemia with diminished awareness during the past year since there were no signs of sympathetic activation. This might obscure other underlying causes of hypoglycemia if patient was not assessed thoroughly. However, his glucose level fluctuated drastically and was very difficult to correct. Further investigation for NICTH is merited given high risk of malignancy.

Figure 1 Arterial phase of abdominal computed tomography showed a centrally necrotic mass in the left hepatic lobe, measuring 6.7 cm × 6.5 cm (orange arrow).

Figure 2 Capillary blood glucose trend.

Two types of NICTH (type A and B) are seen in HCC patients[10]. Type A often occurs at the terminal stage of disease when there is an increased glucose consumption by the tumor on top of a progressive reduction in glucose supply due to hepatic failure on the residual liver tissue and in part due to malnutrition. The tumor mass is usually rapid growing and poorly differentiated, associated with severe anorexia, muscle wasting and weight loss. But hypoglycemia is often mild and relatively easier to correct[11,12]. Type B, less common than type A, is related to an overproduction of IGF-2 and its precursors by the tumor. It often occurs at the earlier course of the disease and is thought to be a paraneoplastic syndrome. The severity of hypoglycemia is predominant and is often difficult to control. Glucose utilization by the tumor might also contribute to the hypoglycemia but is not a significant pathway[9]. The excess of IGF-2 Messenger RNA overwhelms the enzyme transforming pro-IGF-2 to mature IGF-2, thus producing various sizes of incompletely processed and unprocessed pro-IGF-2, the so called “big IGF-2”[3,13]. Normally most of serum IGF-2 is transported in the form of a 150 kDa ternary complex together with insulin-like growth factorbinding protein 3 and acid-labile sub-unit. But the “big IGF-2” mainly forms a 50 kDa binary complex with only insulin-like growth factor-binding protein 3. These binary complexes have a higher biological activity and can readily cross the capillary membrane to interact with insulin receptors in the liver, adipose tissue, and skeletal muscle due to their smaller size, leading to more glucose uptake and inhibition of gluconeogenesis[14,15]. By interacting with the IGF-1 receptors in the hypothalamus, the excess of pro-IGF-2 and IGF-2 inhibits the secretion of growth hormone, which in turn suppresses the production of IGF-1, insulin-like growth factor-binding protein 3, and acid-labile sub-unit. Therefore, more amount of free IGF-2 might gain access to the target tissue[16-19].

As to our patient, IGF-2 was inappropriately normal for the extremely low IGF-1 level. An IGF-2/IGF-1 ratio greater than 10 has been proposed to be enough to confirm the diagnosis of NICTH[16,20,21]. IGF-2 might be falsely normal in our patient because the sample was collected after the first dose of prednisolone was administered, which was able to inhibit the production of IGF-2[22]. In addition, serum IGF-2 levels in NICTH are often not elevated partially because most “big IGF-2” are not measured by common commercially available assay[16,23,24]. It has also been found by a few case reports that the levels of serum IGF-2 were decreased or normal in contrast to an increased pro-IGF-2 in NICTH[25,26]. Pro-IGF-2 was not measured in this patient because the test was not available in our setting. Although we are not able to entirely exclude the possibility of excessive glucose consumption by the tumor, the tumor mass was not extensive, only occupying part of the left lobe, and the level of AFP was not significantly elevated, indicating mild biological activities. The hepatic failure was more likely due to his advanced cirrhosis rather than the tumor. Therefore, we believe that our case fits more into type B rather than type A NICTH.

Priority of management of NICTH is still tumor resection. In inoperable patients, several treatment options of local tumor cytoreduction are recommended, including percutaneous ethanol injection and trans-arterial chemoembolization[27,28]. Systemic chemotherapy, such as Sorafenib or FOLFOX (oxaliplatin and 5-fluorouracil/leucovorin), has also been showed to be effective[29]. In addition, emerging drugs that directly inhibit the IGF signals (PI3K-AKT-TOR or RAF-MEK-ERK) are under investigation[30]. In case that the primary malignancy cannot be treated, palliative medical management can be chosen. Glucocorticoid together with frequent high carbohydrate meals and IV glucose infusions is an ideal option to achieve longterm prevention of hypoglycemia. Glucocorticoid, on one hand, stimulates hepatic gluconeogenesis and inhibits peripheral glucose uptake; on the other hand, can reduce the level of “big IGF-2” either by decreasing tumor production or by promoting the maturation of pro-IGF-2 and the formation of normal ternary complexes[22,31-33]. Other than glucocorticoid, glucagon, growth hormone, and octreotide infusion are also recommended, but their effects are transient and limited[2,8,34,35]. Our patient initially showed responses to high-dose prednisolone, but it failed to last for a long time mainly because of a poor hepatic reserve from cirrhosis. And the concurrent sepsis and pneumonia further destroyed patient’s ability to maintain the euglycemic status.

CONCLUSION

In conclusion, paraneoplastic NICTH should be considered in the evaluation of refractory hypoinsulinemic hypoglycemia in patients with risk factors of HCC, even in the setting of chronic fasting hypoglycemia induced by severe hepatic failure and malnutrition. NICTH can occur as the only initial presentation of HCC. Oral corticosteroids and frequent high carbohydrate meals are often recommended but the outcome is unfavorable in general if tumor removal is not possible.