Prognostic Value of Preoperative Serum Leucine Aminopeptidases in Hepatocellular Carcinoma Patients Who Underwent Liver Transplantation.

BACKGROUND: Leucine aminopeptidases (LAPs) have been reported to be involved in tumor cell proliferation, invasion and angiogenesis. However, the relationship between serum leucine aminopeptidases and prognosis of hepatocellular carcinoma (HCC) patients who underwent liver transplantation (LT) was not yet reported. We aimed to evaluate the prognostic value of preoperative serum leucine aminopeptidases in these patients.
METHODS: Clinical data of 106 HCC patients who underwent LT were retrospectively analyzed. The sex ratio, age, HBV infection, Child-Pugh stage, preoperative tumor therapy, AFP, the largest tumor size, tumor number, Edmondson grading, macro- and micro-vascular invasion of patients with different serum LAP level and compositions of patients who met the criteria of Milan, UCSF or Hangzhou were compared using the chi-square test. The Kaplan-Meier method was performed in survival analysis and the log rank test was used in survival comparison.
RESULTS: Serum LAPs were correlated with alpha-fetoprotein (AFP), the largest tumor size, tumor number and macro-vascular invasion. Patients with serum LAPs > 87 U/L showed significantly poorer disease-free survival (DFS) and overall survival (OS) than those with serum LAPs ≤ 87 U/L. Univariate analysis indicated that serum LAPs, AFP, the largest tumor size, tumor number, and macro- and micro-vascular invasion were all associated with DFS and OS. Multivariate analysis showed that serum LAPs, macro-vascular invasion and the largest tumor size were independently correlated with DFS and OS. Serum LAPs could also distinguish prognosis between patients with different status of AFP, the largest tumor size, tumor number, and macro- and micro-vascular invasion, as well as patients within and beyond selection criteria, such as Milan, University of California, San Francisco and Hangzhou criteria.
CONCLUSION: Elevated preoperative serum LAPs were associated with advanced tumor stage and aggressive biological behavior, and thus a poor outcome, which could be a prognostic marker for HCC patients who underwent LT.

Introduction

Liver cancer was the sixth most common cancer worldwide in terms of 792,000 new diagnosed cases, and the third most common cause of death from cancer (818,000 deaths annually).1 Despite the progress of hepatitis B virus (HBV) vaccine prevention and treatment options for liver cancer, the cancer burden is increasing owing to the population growing and aging.1 Eighty-six percent of liver cancer occurred in developing countries and 90% were hepatocellular carcinoma (HCC).2 Nowadays, liver transplantation (LT) has been one of the options to cure HCC radically accompanied by liver resection, radiofrequency ablation, microwave ablation, percutaneous ethanol injection and so on.3 Compared with other radical treatment, LT removed the cirrhotic liver4 and a well-controlled HBV recurrence,5 patients could benefit more from this operation theoretically and practically.6–9 However, there are still a proportion of HCC patients who underwent LT suffering from tumor recurrence even when they met the selection criteria, such as Milan criteria,10 University of California, San Francisco (UCSF) criteria11 and Hangzhou criteria.12

Because of the organ shortage for LT, it is increasingly important to achieve the maximum benefit of LT for HCC patients. Previously, some studies have proven the deficiency of the well-acknowledged criteria, including Milan criteria, UCSF criteria and Hangzhou criteria, and some new combined criteria had been brought up.13–18 Some of these combined criteria included objective biological criteria, irrelevant to age, gender, pathology and so on, so they are more reproducible.13,14,19 On the other hand, the criteria for the diagnosis of HCC have improved as well and serum enzymes are taking an increasingly important part. Leucine aminopeptidases (LAPs), a diverse set of exopeptidases, catalyze the hydrolysis of leucine residues from the amino-termini of protein or peptide substrates.20 To be mentioned, LAPs have distinct substrate specificities beyond Leu hydrolysis with different temperature, pH and divalent cation requirements. Some LAPs could act as transcription factors, participate in specific recombination or interact with key membrane transporters.21 They have been demonstrated in most human tissues and high activities in the liver, duodenum, small intestine, pancreas, testis and stoma cells of the uterus.22 LAPs also have been reported related to malignant cell proliferation, invasion and angiogenesis,21,23,24 and implicated in the pathological disorder of livers.21,23,25 Besides, the expression of LAPs is interrelated to prognosis and malignant development of HCC.26,27 However, the prognostic value of serum LAPs on patients with HCC who underwent liver transplantation has not been reported. We aimed to evaluate the prognostic value of preoperative serum leucine aminopeptidases in these patients.

Patients and Methods

All the preoperative clinical data of HCC patients who underwent liver transplantation at the Organ Transplant Center, the First Affiliated Hospital, Sun Yat-sen University from March, 2005 to October, 2013 were collected. Patients with hepatorenal syndrome on hemodialysis, uncontrolled severe infection, HIV infection, other uncured malignant tumor, HCC metastases beyond the liver, hepatic and portal vein invasion and without preserved lung and cardiac function to tolerate LT were excluded from the waiting list. The diagnosis was confirmed through hematoxylin–eosin staining and immunohistochemistry (when necessary) by at least two pathologists. All the patients received deceased donor liver transplantation. All organs were donated voluntarily with written informed consent, and this was conducted in accordance with the Declaration of Istanbul. The retrospective study was approved by the medical ethic committee of the First Affiliated Hospital, Sun Yat-sen University in compliance with the Declaration of Helsinki, and the ethic approval number was [2016]081. Due to the retrospective nature of the study, written informed consent was waived. Data confidentiality was assured by storage of patient identifiers in separate encrypted files and the files were accessible only to the research team offline. Only the patients with complete preoperative clinical, laboratory, imaging and follow-up data were selected. The general status of patients, such as gender, age, HBsAg, Child–Pugh stage and preoperative tumor therapy, was used to evaluate the comparability between groups, and tumor-related markers, such as serum AFP, the largest tumor size, tumor number, Edmondson grading, and macro- and micro-vascular invasion, were compared between patients with different LAP levels.

Experimental Design

The patients were classified based on the cutoff value, which was selected using the receiver operating characteristic (ROC) curve analysis. A combination of Milan criteria or UCSF criteria or Hangzhou criteria and LAP cutoff value were used to classify HCC patients into four groups: patients who met the criteria and LAP level below the cutoff value, patients who met the criteria and LAP level above the cutoff value, patients beyond the criteria and LAP level below the cutoff value, and patients beyond the criteria and LAP level above the cutoff value.

Treatment and Follow-Up

All the patients received modified piggy-back orthotopic liver transplantation or classic orthotopic liver transplantation. Perioperative treatment and follow-up were as described previously.28 Briefly, two doses of 20 mg basiliximab (Simulect, Novartis Pharma AG, Basel, Switzerland) were given intraoperatively and the fourth day after surgery. Mycophenolate mofetil (MMF) and FK506 were used post surgery to prevent organ rejection. The concentration of FK506 was tested routinely and adjusted according to the test results and serum liver enzyme level, and the serum creatinine level was also taken into consideration. Blood routine tests, liver enzyme level, and serum tests of hepatic and renal function were performed at each follow-up, and also for serum AFP level and liver ultrasound test. An abdominal CT scan was performed every 6 months. Clinical and radiological manifestations of tumor, with or without pathological diagnosis,29 were defined as tumor recurrence. As for the patients suffering from recurrence, radiofrequency ablation (RFA), transarterial chemoembolization (TACE), sorafenib administration, tumor resection and chemotherapy were chosen based on the patient’s specific condition.

Statistical Analysis

Statistical analysis was performed using SPSS software (Windows Version 16.0; SPSS Inc., Chicago, IL, USA). The ROC curve analysis was used to determine the optimal cutoff value of LAPs. The demographic and clinicopathological data were compared between HCC patients with low and high LAP values using the chi-square test. Survival analysis was performed using the Kaplan–Meier method and compared using the log rank test. A multivariate Cox regression model using a forward (conditional) method was used to identify independent risk factors that affected patients’ survival. P value less than 0.05 was considered statistically significant.

Results

Clinicopathological Characteristics of Patients

A total of 106 HCC patients were enrolled in this study, including 100 male patients and 6 female patients with a median age of 49 (range from 13 to 66) years. Median follow-up time was 38 months. Half of these patients suffered from tumor recurrence, and 40 patients died of tumor progression. One hundred and one out of the 106 patients were infected by HBV. According to the Child–Pugh score system, 67 patients were within Child–Pugh stage A, and 29 and 10 for Child–Pugh stage B and C, separately (). Forty-nine patients received preoperative therapy, such as hepatectomy, radiofrequency ablation and transcatheter arterial chemoembolization (). There were 67 patients of grading I–II and 39 patients of grading III–IV according to Edmondson–Steiner grading. Moreover, patients were classified through three well accepted criteria: Milan criteria, UCSF criteria and Hangzhou criteria. Thirty-seven patients fulfilled the Milan criteria, 56 patients for UCSF criteria and 66 patients for Hangzhou criteria.

The Determination of Serum LAP Cutoff Value and Its Sensitivity and Specificity

The best cutoff value of serum LAPs was 87 U/L by the ROC curve (), and the sensitivity and specificity were 0.736 and 0.755 (the area under the ROC curve: 0.788, 95% confidence interval: 0.699–0.877, P < 0.001), separately.

Clinical Character of Hepatocellular Carcinoma Patients with Different Serum LAP Value

All the enrolled patients were divided into two groups based on the serum LAP cutoff value, and clinical character was compared between groups (Table 1). There was no significant difference in general status between the two groups, such as gender, age, serum hepatitis B virus antigen (HBsAg) positive rate, Child–Pugh classification and preoperative therapy, indicating the comparability between the two groups. Patients with serum LAPs > 87 U/L tended to have higher serum alpha-fetoprotein (AFP) level, larger tumor size, more tumor nodules and higher rate of macro-vascular invasion. In addition, patients with serum LAPs > 87 U/L tended to exceed the Milan, UCSF and Hangzhou criteria.

Table 1

Comparison of Clinical Character Between HCC Patients Who Underwent Liver Transplantation with Different Serum LAPs

Category	Subcategory	Cases	LAPs (U/L)		P value
			≤87 (n = 54)	>87 (n = 52)
Gender	Male	100	49	51
	Female	6	5	1	0.102
Age (years)	≤50	56	27	29
	>50	50	27	23	0.552
HBsAg	Positive	101	51	50
	Negative	5	3	2	0.678
Child–Pugh stage	A	67	35	32
	B	29	15	14
	C	10	4	6	0.767
Preoperative tumor therapy	Yes	49	26	23
	No	57	28	29	0.686
AFP (ng/mL)	≤400	69	44	25
	>400	37	10	27	<0.001
The largest tumor size (cm)	≤5	61	41	20
	5 to 8	19	7	12
	>8	26	6	20	<0.001
Tumor number	≤3	74	43	31
	>3	32	11	21	0.025
Edmondson grading	I–II	67	36	31
	III–IV	39	18	21	0.452
Macro-vascular invasion	Yes	27	5	22
	No	79	49	30	<0.001
Micro-vascular invasion	Yes	13	3	10
	No	93	42	51	0.131
Milan criteria	Within	37	30	7
	Beyond	69	24	45	<0.001
UCSF criteria	Within	56	39	17
	Beyond	50	15	35	<0.001
Hangzhou criteria	Within	66	45	21
	Beyond	40	9	31	<0.001

Disease-Free Survival and Overall Survival Comparison Between Patients with Different Serum LAP Value

The prognosis of HCC patients with different levels of serum LAPs was evaluated using Kaplan–Meier survival analysis (Figure 1), and compared using the log rank test. The 1, 3, 5-year DFS rates were significantly poorer for patients with serum LAPs > 87 U/L (n = 52) than patients with serum LAPs ≤ 87 U/L (n = 54) (50.0%, 28.8%, 19.2% vs 87.0%, 77.5%, 72.1%, P < 0.001), which was also the same for 1, 3, 5-year OS rates between the two groups (71.2%, 41.6%, 35.8% vs 98.1%, 87.0%, 82.3%, P < 0.001). Then, further investigation was performed based on the LAP level. The patients were divided into three groups: group 1, patients with serum LAPs ≤ 87 U/L (n = 54), the cutoff value and which was close to the normal range of serum LAPs (30~70 U/L). The other patients were classified into another two groups by the median of serum LAP level (123 U/L), which were group 2 for patients with serum LAPs between 87 and 123 U/L (n = 27) and group 3 for patients with serum LAPs > 123 U/L (n = 25). The patients’ DFS and OS were also analyzed through the Kaplan–Meier method and compared using the log rank test. The 1,3,5-year DFS rates for patients in group 1 were 87.0%, 77.5% and 72.1%, separately, 66.7%, 44.4% and 38.1% for group 2 patients, and 32.0%, 12.0% and 6.0% for group 3 patients. All the P values between any two groups were less than 0.05 (0.002 for group 1 vs group 2, <0.001 for group1 vs group 3 and 0.003 for group 2 vs group 3). Accordingly, the 1, 3, 5-year OS rates were 98.1%, 87.0% and 82.3% for group 1, 81.5%, 57.6% and 52.8 for group 2, and 60.0%, 23.0% and 17.2% for group 3, separately. All the differences between groups were also statistically significant (0.006 for group 1 vs group 2, <0.001 for group1 vs group 3 and 0.005 for group 2 vs group 3). A bivariate analysis using Pearson’s correlation was conducted to evaluate the correlation between serum LAPs and DFS or OS, and found that the correlation coefficient between LAPs and DFS was −0.417 (P < 0.001), and −0.375 for LAPs and OS (P < 0.001). Besides the prognostic value of serum LAPs, there was also a negative correlation between its level and prognosis; the higher the serum LAP value, the worse the prognosis.

Figure 1

DFS and OS for HCC patients who underwent liver transplantation with different levels of serum LAPs. DFS and OS of patients with lower serum LAPs were significantly better than those with higher serum LAPs.

Clinicopathological Data on Patients’ Prognosis

Univariate analysis indicated that serum LAPs, AFP level, the largest tumor size, tumor number, macro-vascular invasion and micro-vascular invasion were all related with patients’ prognosis (Table 2). HCC patients with AFP > 400 ng/mL, the larger tumor size, tumor number > 3, macro-vascular invasion and micro-vascular invasion had a significant worse outcome than those without such characters. Then, the positive variables were added to the multivariate Cox regression model directly, except for the variable the largest tumor size, which was added after being transformed as the largest tumor size ≤ 5 cm or > 5 cm and ≤ 8 cm or > 8 cm, to screen the independent risk factor on patients’ prognosis. Macro-vascular invasion, the largest tumor size > 5 cm and serum LAP level > 87 U/L were independent factors that significantly affected patients’ prognosis (Table 3).

Table 2

Clinicopathological Variables Affecting Prognosis in HCC Patients Who Underwent Liver Transplantation

Variables	n	DFS				OS
		1-Yr	3-Yr	5-Yr	P	1-Yr	3-Yr	5-Yr	P
Age (years)
≤50	56	62.5%	47.9%	43.3%		78.6%	58.2%	52.8%
>50	50	76.0%	60.0%	50.6%	0.225	92.0%	73.0%	67.2%	0.121
Child–Pugh stage
A	67	64.2%	46.1%	37.1%		82.1%	60.6%	54.2%
B	29	75.9%	62.1%	55.9%		89.7%	70.2%	65.1%
C	10	80.0%	80.0%	80.0%	0.067	80.0%	80.0%	80.0%	0.326
Preoperative tumor therapy
Yes	49	73.5%	50.8%	38.6%		87.8%	68.6%	58.5%
No	57	64.9%	56.1%	50.2%	0.775	82.5%	62.2%	59.8%	0.776
AFP (ng/mL)
≤400	69	82.6%	69.3%	60.1%		92.8%	79.2%	75.3%
>400	37	43.2%	24.3%	20.3%	<0.001	70.3%	38.5%	31.4%	<0.001
The largest tumor size (cm)
≤5	61	86.9%	75.4%	70.7%		96.7%	86.0%	83.6%
5 to 8	19	68.4%	36.1%	24.1%		78.9%	57.9%	37.1%
>8	26	26.9%	15.4%	10.3%	<0.001	61.5%	23.1%	23.1%	<0.001
Tumor number
≤3	74	79.7%	67.4%	58.8%		86.5%	78.1%	69.8%
>3	32	43.8%	21.9%	17.5%	<0.001	81.2%	34.9%	34.9%	<0.001
Edmondson grading
I–II	67	71.6%	53.4%	47.8%		88.1%	70.5%	60.8%
III–IV	39	64.1%	53.8%	44.3%	0.817	79.5%	56.1%	56.1%	0.285
Macro-vascular invasion
Yes	27	40.7%	7.4%	3.7%		66.7%	25.9%	17.3%
No	79	78.5%	69.6%	61.4%	<0.001	91.1%	80.6%	74.3%	<0.001
Micro-vascular invasion
Yes	13	38.5%	7.7%	7.7%		69.2%	30.8%	23.1%
No	93	73.1%	59.1%	52.3%	<0.001	87.1%	70.2%	65.0%	0.001
Milan criteria
Within	37	91.9%	89.2%	84.9%		97.3%	94.5%	94.5%
Beyond	69	56.5%	345%	25.7%	<0.001	78.3%	49.4%	41.3%	<0.001
UCSF criteria
Within	50	91.1%	81.8%	79.0%		94.6%	91.0%	86.2%
Beyond	56	44.0%	22.0%	10.9%	<0.001	74.0%	36.6%	30.9%	<0.001
Hangzhou criteria
Within	66	84.8%	78.8%	72.0%		92.4%	86.1%	84.0%
Beyond	40	42.5%	12.5%	4.7%	<0.001	72.5%	30.9%	21.7%	<0.001

Table 3

Independent Risk Factors for Prognosis in HCC Patients Who Underwent Liver Transplantation

Variables	DFS			OS
	HR	95% CI	P	HR	95% CI	P
Macro-vascular invasion	2.480	1.327–4.633	0.004	2.401	1.185–4.863	0.015
LAPs	2.659	1.371–5.156	0.004	2.479	1.100–5.587	0.029
The largest tumor size	2.514	1.306–4.838	0.006	3.627	1.584–8.301	0.002

As previous described, the AFP level, the largest tumor size, tumor number, macro-vascular invasion and micro-vascular invasion, along with LAP level, were related with patients’ prognosis, and then we evaluated the distinguishing value of serum LAPs in patients with or without these conditions using the Kaplan–Meier method and compared using the log rank test.

Distinguishing Effect of LAPs in HCC Patients with Different Level of AFP

For patients with AFP ≤ 400 ng/mL, the 1, 3, 5-year DFS rates were significantly poorer for these with serum LAPs > 87 U/L (n = 25) than those with serum LAPs ≤ 87 U/L (n = 44) (72.0%, 52.0%, 34.7% vs 88.6%, 79.2%, 72.5%, P = 0.017), which was the same for patients’ OS rates (80.0%, 62.1%, 56.5% vs 100%, 88.6%, 85.8%, P = 0.009). Accordingly, for patients with AFP > 400 ng/mL, the 1, 3, 5-year DFS rates were also poorer for these with serum LAPs > 87 U/L (n = 27) than those with serum LAPs ≤ 87 U/L (n = 10) (29.6%, 7.4%, 3.7% vs 80.0%, 70.0%, 70.0%, P < 0.001), and also there was the same condition in OS comparison (70.4%, 21.5%, 17.2% vs 90.0%, 80.0%, 68.6%, P = 0.009) (Figure 2).

Figure 2

DFS and OS for HCC patients who underwent liver transplantation with AFP ≤ 400 ng/mL and > 400 ng/mL grouped by serum LAP level.

Distinguishing Effect of LAPs in HCC Patients with Different Size of the Largest Tumor

As previously described, the largest tumor size > 5 cm was the independent risk factor on patients’ prognosis, and then we investigated the prognostic value of serum LAPs in patients with different tumor size. For patients with the largest tumor size ≤ 5 cm, the 1, 3, 5-year DFS rates were significantly poorer in patients with serum LAPs > 87 U/L (n = 20) than in those with serum LAPs ≤ 87 U/L (n = 41) (80.0%, 50.0%, 50.0% vs 90.2%, 87.8%, 80.7%, P = 0.007), which was also similar in patients’ 1, 3, 5-year OS rates (95.0, 64.9%, 56.8% vs 97.6%, 95.1%, 95.1%, P = 0.001). For patients with the largest tumor size > 5 cm, the 1, 3, 5-year DFS rates were significantly poorer for those with serum LAPs > 87 U/L (n = 32) than those with serum LAPs ≤ 87 U/L (n = 13) (31.2%, 15.6%, 7.8% vs 76.9%, 46.2%, 46.2%, P = 0.008). There was the same trend in patients’ 1, 3, 5-year OS rates (95.0, 64.9%, 56.8% vs 97.6%, 95.1%, 95.1%, P = 0.095), but not statistically significant (Figure 3).

Figure 3

DFS and OS for HCC patients who underwent liver transplantation with the largest tumor size ≤ 5 cm and > 5 cm grouped by serum LAP level.

Distinguishing Effect of LAPs in HCC Patients with Different Tumor Number

For patients with tumor number ≤ 3, the 1, 3, 5-year DFS rates were significantly poorer for patients with serum LAPs > 87 U/L (n = 31) than those with serum LAPs ≤ 87 U/L (n = 43) (61.3%, 45.2%, 26.3% vs 93.0%, 83.4%, 79.8%, P < 0.001). And it was the same for patients’ OS rates (71.0%, 60.2%, 49.4% vs 97.7%, 90.7%, 84.8%, P < 0.001). For patients with tumor number > 3, the 1, 3, 5-year DFS rates were significantly poorer for patients with serum LAPs > 87U/L (n =2 1) than those with serum LAPs ≤ 87U/L (n = 11) (33.3%, 4.8%, 4.8% vs 63.6%, 54.5%, 40.9%, P = 0.010). And it was the same for patients’ OS rates (74.4%, 15.4%, 15.4% vs 100%, 72.7%, 72.7%, P = 0.006) (Figure 4). No matter whether the tumor number was more than 3, patients with serum LAPs > 87 U/L tended to have a poor prognosis.

Figure 4

DFS and OS for HCC patients who underwent liver transplantation with tumor number ≤ 3 and > 3 grouped by serum LAP level.

Distinguishing Effect of LAPs in HCC Patients without and with Macro-Vascular Invasion

As for patients without macro-vascular invasion, the 1, 3, 5-year DFS rates were significantly poorer for these with serum LAPs > 87 U/L (n = 30) than those with serum LAPs ≤ 87 U/L (n = 49) (63.3%, 46.7%, 27.2% vs 87.8%, 83.7%, 80.5%, P < 0.001). And it was the same for patients’ OS rates (80.0%, 64.7%, 53.1% vs 98.0%, 89.8%, 87.2%, P = 0.002). For patients with macro-vascular invasion, the 1, 3, 5-year DFS and OS were poorer for these with serum LAPs > 87 U/L (n = 22) than those with serum LAPs ≤ 87 U/L (n = 5), but not statistically significant (31.8%, 4.5%, 0 vs 80.0%, 20.0%, 0 for 1, 3, 5-year DFS rates, P = 0.136). And it was the same for patients’ OS rates (59.1%, 13.6%, 0 vs 100%, 60.0%, 30.0% for 1, 3, 5-year OS, P = 0.162) (). Serum LAPs could be a prognostic marker for patients without macro-vascular invasion, but not for patients with macro-vascular invasion.

Distinguishing Effect of LAPs in HCC Patients without and with Micro-Vascular Invasion

As for patients without micro-vascular invasion, the 1, 3, 5-year DFS rates were significantly poorer for these with serum LAPs > 87 U/L (n = 42) than those with serum LAPs ≤ 87 U/L (n = 51) (54.8%, 33.3%, 29.2% vs 88.2%, 80.4%, 77.7%, P < 0.001). And it was the same for patients’ OS rates (73.8%, 47.5%, 39.7% vs 98.0%, 88.2%, 85.6%, P < 0.001). For patients with micro-vascular invasion, the 1, 3, 5-year DFS and OS rates were poorer for these with serum LAPs > 87 U/L (n = 10) than those with serum LAPs ≤ 87 U/L (n = 3), but not statistically significant (30.0%, 10.0%, 10.0% vs 66.7%, 33.3%, 0 for 1, 3, 5-year DFS, P = 0.292). And it was the same for patients’ OS rates (60.0%, 20.0%, 20.0% vs 100%, 66.7%, 33.1% for 1, 3, 5-year OS rates, P = 0.425) ().

Distinguishing Effect of LAPs in HCC Patients Within and Beyond Selection Criteria

Serum LAPs had been demonstrated to be a prognostic marker for patients with different AFP level, tumor number, tumor size ≤ 5 cm, no macro-vascular invasion and no micro-vascular invasion. Then, we investigated the prognostic value of serum LAPs in patients within and beyond three well accepted criteria, Milan criteria, UCSF criteria and Hangzhou criteria, all of which were combinations of tumor size, tumor number, tumor size and AFP level. For patients who met Milan criteria, the 1, 3, 5-year DFS rates for these with serum LAPs > 87 U/L (n = 7) were significantly poorer than those with serum LAPs ≤ 87 U/L (n = 30) (71.4%, 57.1%, 57.1% vs 96.7%, 96.7%, 91.3%, P = 0.007), which were also the same for patients beyond Milan criteria. The 1, 3, 5-year DFS rates for patients with serum LAPs > 87 U/L (n = 45) were significantly poorer than patients with serum LAPs ≤ 87 U/L (n = 24) (46.7%, 24.4%, 14.0% vs 75.0%, 53.5%, 47.5%, P = 0.010). For patients who met UCSF criteria, the 1, 3, 5-year DFS rates for these with serum LAPs > 87 U/L (n = 17) were poorer than those with serum LAPs ≤ 87 U/L (n = 39), but not statistically significant (82.4%,70.6%, 70.6% vs 94.9%, 86.8%, 82.7%, P = 0.188), which may due to a relative small difference between the groups and limited patients enrolled. However, for patients beyond UCSF criteria, the 1, 3, 5-year DFS rates for these with serum LAPs > 87 U/L (n = 35) were significantly poorer than those with serum LAPs ≤ 87 U/L (n = 15) (34.3%, 8.6%, 2.9% vs 66.7%, 53.3%, 44.4%, P = 0.002). For patients within and beyond Hangzhou criteria, the 1, 3, 5-year DFS rates were significantly poorer for these with serum LAPs > 87 U/L than those with serum LAPs ≤ 87 U/L. For patients who met Hangzhou criteria, the 1, 3, 5-DFS rates were 76.2%, 61.9%, 41.3% and 88.9%, 86.7%, 83.2% for patients with serum LAPs > 87 U/L (n = 21) and ≤ 87 U/L (n = 45), separately. For patients beyond Hangzhou criteria, which were 32.3%, 6.5%, 3.2% and 77.8%, 33.3%, 16.7% for patients with serum LAPs > 87 U/L (n = 31) and ≤ 87 U/L (n = 9), separately, the P values were 0.015 and 0.034 (Figure 5) ().

Figure 5

DFS for HCC patients who underwent liver transplantation within and beyond selection criteria grouped by serum LAP level.

Discussion

We demonstrated, for the first time, that serum LAPs could be an important prognostic marker for HCC patients who underwent LT. These patients with elevated serum LAPs (>87 U/L) showed a higher rate of tumor recurrence and shorter lifespan, and further investigation indicated that there was negative correlation, to some extent, between serum LAP level and HCC patients’ prognosis both on DFS and OS. It was also found that patients with serum LAPs > 87 U/L tended to have higher serum AFP level, larger tumor size, more tumor nodules and higher rate of macro-vascular invasion, which were all related to poor prognosis. Multivariate analysis revealed that serum LAPs > 87 U/L, accompanied by the largest tumor size > 5 cm and macro-vascular invasion, was an independent risk factor for prognosis both on DFS and OS. Serum LAPs also showed a distinguishing effect in patients with different status of AFP level, tumor number, the largest tumor size ≤ 5 cm, no macro-vascular invasion and no micro-vascular invasion. As for patients who met the criteria of Milan, UCSF and Hangzhou criteria, the prognosis both on DFS and OS of patients with LAPs ≤ 87 U/L was significantly better than those with LAPs > 87 U/L, except for patients who met the criteria of USCF.

The exact mechanism of LAPs on tumor malignancy had been investigated. As previously described, LAPs contained many subsets, leucine aminopeptidase 3, a member of LAPs from the peptidase M17 family, whose expression was significantly up-regulated in HCC tissues and cell lines compared with normal liver tissues and human hepatocyte cell line, separately.26 LAP3 promoted HCC cell line proliferation by regulating the G1/S checkpoint in the cell cycle and facilitate cell migration, which were correlated with lower differentiation, positive lymph node metastasis, high Ki-67 expression and a poor OS rate in HCC patients.26 It was also demonstrated in ovarian cancer cells that LAP3 regulated P38 MAPK/Hsp27 and PI3K/Akt pathways and was associated with the expression of fascin and MMP-2/9 protein, which played important roles in tumor cell migration and extracellular matrix degradation.30 As for human gliomas, increased LAP3 expression was associated with the tumor degrading and poor OS, and could facilitate glioma cell viability, proliferation, migration and invasion in vitro.31 Similar results were found in patients with esophageal squamous cell carcinoma and cell lines.32

Other subsets of LAPs, aminopeptidase N (APN or CD13) and adipocyte-derived leucine aminopeptidase/puromycin insensitive leucyl-specific aminopeptidase, members of LAPs from the peptidase M1 family, were reported to participate in angiogenesis, which may partially explain the high incidence of macro-vascular invasion in patients with higher serum LAP level. APN/CD13 had been reported to be associated with extracellular matrix degradation and thus to facilitate tumor invasion.33,34 Immunohistochemical staining showed that APN was expressed in the vasculature of carcinoma both in human and experimental animals and in corpus luteum undergoing angiogenesis, as was negative in blood vessels of normal tissues.35 Both APN antibodies and leucine aminopeptidase inhibitor could inhibit neovascularization and tumor growth.35 Further investigation showed that the RAS/MAPK pathway and phosphatidylinositol-3 kinase were involved in the induction of CD13/APN expression in response to angiogenic growth factors through up-regulation of CD13/APN promoter activity.36,37 The proto-oncogene c-Maf could also potently activate transcription of the CD13 through directly binding the −153 bp promoter region.38 A mouse orthologue of PILSAP, another type of LAP, had been demonstrated to be expressed in endothelial cells during postnatal angiogenesis and be of importance in angiogenesis both in vitro and in vivo.39

Besides, placental leucine aminopeptidase (P-LAP), also a member of leucine aminopeptidases from the aminopeptidase M1 family, is membrane-bound and transported through vesicles, which could be cleaved proteolytically by metalloproteases and form the serum P-LAP. P-LAP, distributed widely in human tissues, other than being limited to the placenta only, which participated in physiological activities, such as pregnancy,40 diabetes41 and blood pressure,42 had also been reported to be involved in malignancy.43 In patients with endometrial carcinoma, tissue expression of P-LAP could serve as an independent prognostic marker of clinical outcome, and was positively associated with tumor histological grade, surgical stage, myometrial invasion, lymph node involvement, vascular infiltration and poor disease-free interval.44 Similar results were also found in rat breast cancer tissues.45

All of these research studies mentioned above were focused on tissue and cell LAP expression, and serum LAPs could be cell-derived enzymes with or without molecular aggregates.24 Elevated serum LAPs in HCC patients have been reported by investigators domestic and abroad,27,46,47 which also could serve as a tumor marker in HCC diagnosis27 and differentiation from secondary hepatocarcinoma,47 but its prognostic value in HCC patients who underwent LT was not yet reported. Besides HCC, serum LAP elevation was also found in patients with chronic granulocytic leukemia, acute myelocytic leukemia, myelofibrosis, lymphosarcoma and malignant melanoma.24 As for patients enrolled in the study, none of these diseases coexisted.

There were several limitations for this study; as a routine biochemical test, we evaluated the total activity of LAPs without further tests of its subsets. No specific subsets of LAPs were tested either in serum or hepatocellular carcinoma tissues. There were also other shortages, such as the small enrolled population, certain proportion of data censored, less convincing than prospective studies due to the nature of its retrospective analysis and potentially confounding factors caused by donor characteristics. However, due to its ethical reason, a prospective study may not be available until more evidence based on an enlarged HCC population from multiple liver transplantation centers confirms the prognostic value of LAP.

In conclusion, serum LAPs could be a prognostic marker for HCC patients who underwent LT, and patients with elevated serum LAPs tended to have higher AFP level, larger tumor size, more tumor nodules, more macro-vascular invasion and thus a poor outcome both on DFS and OS. Further investigation revealed a negative correlation between serum LAP level and patients’ DFS and OS. Serum LAPs could be used to screen patients more suitable for LT and with high risk of tumor recurrence both within and beyond the three well known criteria, except for patients within UCSF criteria. The exact mechanism of serum LAPs or its subset on tumor malignancy and HCC patients’ prognosis is still in need of further investigation.