Abstract

Background Circulating apolipoprotein-AII (apoAII-) ATQ/AT is a potential useful biomarker for early stage pancreatic ductal adenocarcinoma (PDAC), but its clinical significance in PDAC patients remains uncertain. The aim of the current study was to assess the usefulness of apoAII-ATQ/AT as a surrogate for the effect of chemoradiotherapy (CRT) and its association with pancreatic exocrine disorder, paying attention to morphological changes of the pancreas. Methods In the 264 PDAC patients who were enrolled in our CRT protocol, the following parameters were measured at specified time points before and after CRT: serum levels of albumin, total cholesterol, and amylase as indices of pancreatic exocrine function, serum levels of CA19-9, and the pancreatic morphology including tumor size (TS), main pancreatic duct diameter (MPDD), and pancreatic parenchymal volume excluding tumor volume (PPV) by using computed tomography (CT) images. Plasma apoAII-ATQ/AT levels were simultaneously measured with enzyme-linked immunosorbent assay in 4 healthy volunteers and the 44 PDAC patients before and after CRT. Plasma apoAII-ATQ/AT levels after CRT were analyzed according to small/large-MPDD and small/large-PPV groups based on their median values after CRT. Plasma samples after CRT were measured after incubation with human pancreatic juice (PJ) to examine the relevance between apoAII isoforms and circulating pancreatic enzymes. Results The serum levels of albumin, amylase, CA19-9, TS, MPDD, and PPV after CRT were significantly lower than those before CRT (median, before vs. after: 3.9 g/dl, 74 U/l, 180.2 U/ml, 58.1 mm, 4.0 mm, and 34.8 ml vs. 3.8, 59, 43.5, 55.6, 3.6, and 25.2). ApoAII-ATQ/AT levels (median, μg/ml) of PDAC patients before CRT were significantly lower than those in healthy volunteers: 32.9 vs. 61.2, and unexpectedly those after CRT significantly decreased: 14.7. The reduction rate of apoAII-ATQ/AT was not correlated with those of CA19-9 and TS, indicating that apoAII-ATQ/AT is not a tumor-specific marker. On the other hand, the patient group with large MPDD and small PV exhibited higher apoAII-ATQ levels than those with small MPDD and large PPV. The incubation of plasma samples after CRT with PJ did not alter apoAII-ATQ/AT and apoAII-AT levels but significantly decreased apoAII-ATQ levels, suggesting that circulating pancreatic enzymes markedly influenced apoAII-ATQ levels. Conclusions ApoAII-ATQ/AT levels are not useful for evaluation of clinical effect of CRT for PDAC, but apoAII isoforms are very useful to assess pancreatic exocrine disorder because pancreatic atrophy and insufficient secretion of circulating pancreatic enzymes are considered likely to influence apoAII-ATQ levels.

Highlights

  • Pancreatic ductal adenocarcinoma (PDAC) is one of the most lethal malignant tumors

  • The current study revealed that the distribution of apoAII isoforms showed drastic changes between before and after CRT for the pancreatic ductal adenocarcinoma (PDAC) patients, which were not correlated with treatment effect of CRT but rather with the changes in morphological features of the pancreas

  • As the previous studies had already demonstrated, the plasma apoAII-ATQ/AT levels [represented as the plasma apoAII√(ATQ∗AT)] in the current study were significantly lower in the PDAC patients than in the healthy controls, suggesting that apoAII-ATQ/AT is a promising marker for detection of PDAC [2, 3]

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Summary

Introduction

Pancreatic ductal adenocarcinoma (PDAC) is one of the most lethal malignant tumors. Of those afflicted, 10-20% are eligible for potentially curative resection, and up to 80% of patients present with locally advanced or metastatic disease at diagnosis [1]. Circulating apolipoprotein-AII (apoAII-) ATQ/AT is one of the apoAII isoforms and a potential biomarker for screening patients for early stage PDAC. It was previously reported that the levels of apoAII-ATQ/AT in plasma samples from PDAC patients were significantly lower than those from healthy controls [2]. Circulating apolipoprotein-AII (apoAII-) ATQ/AT is a potential useful biomarker for early stage pancreatic ductal adenocarcinoma (PDAC), but its clinical significance in PDAC patients remains uncertain. Plasma apoAII-ATQ/AT levels were simultaneously measured with enzymelinked immunosorbent assay in 4 healthy volunteers and the 44 PDAC patients before and after CRT. ApoAII-ATQ/AT levels are not useful for evaluation of clinical effect of CRT for PDAC, but apoAII isoforms are very useful to assess pancreatic exocrine disorder because pancreatic atrophy and insufficient secretion of circulating pancreatic enzymes are considered likely to influence apoAII-ATQ levels

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