| Literature DB >> 23197977 |
Kiyohito Kato1, Hideki Kamada, Takayuki Fujimori, Yuuichi Aritomo, Masahiro Ono, Tsutomu Masaki.
Abstract
We review the utility of endoscopic ultrasound-guided fine needle aspiration (EUS-FNA), a rapid, safe, cost-effective, and accurate diagnostic modality for evaluating pancreatic tumors. EUS-FNA is currently used for the diagnosis and staging of pancreatic tumors. The sensitivity of EUS-FNA for pancreatic malignancy ranges from 75% to 94%, and its specificity approaches 100% in most studies. However, EUS-FNA has some limitations in the diagnosis of well-differentiated or early-stage cancers. Recent evidence suggests that molecular biological analysis using specimens obtained by EUS-FNA improves diagnostic sensitivity and specificity, especially in borderline cytological cases. It was also reported that additional information regarding patient response to chemotherapy, surgical resectability, time to metastasis, and overall survival was acquired from the genetic analysis of specimens obtained by EUS-FNA. Other studies have revealed that the analysis of KRAS, MUC, p53, p16, S100P, SMAD4, and microRNAs is helpful in making the diagnosis of pancreatic carcinoma. In this paper, we describe the present state of genetic diagnostic techniques for use with EUS-FNA samples in pancreatic diseases. We also discuss the role of molecular biological analyses for the diagnosis of pancreatic carcinoma.Entities:
Year: 2012 PMID: 23197977 PMCID: PMC3503278 DOI: 10.1155/2012/243524
Source DB: PubMed Journal: Gastroenterol Res Pract ISSN: 1687-6121 Impact factor: 2.260
Relationship between cytopathologic evaluation and KRAS point mutation in specimens of pancreatic cancer (62 cases) obtained by EUS-FXA; citation from [7].
| Cytology | KRAS point mutation positive | |
|---|---|---|
| No malignancy | 4 | 2 (50%) |
| Suspicion of malignancy | 7 | 5 (71%) |
| Malignancy | 51 | 39 (76%) |
|
| ||
| Total | 62 | 46 |
Relationship between histopathologic evaluation and KRAS point mutation in specimens of pancreatic cancer (62 cases) obtained by EUS-FXA; citation from [7].
| Histology | KRAS point mutation positive | |
|---|---|---|
| Insufficient material | 7 | 3 (43%) |
| No malignancy | 11 | 7 (64%) |
| Atypical | 5 | 4 (80%) |
| Suspicion of malignancy | 15 | 12 (80%) |
| Malignancy material | 24 | 20 (83%) |
|
| ||
| Total | 62 | 46 |
Accuracy of the 3 tests for diagnosing pancreatic cancer; citation from [16].
| Diagnosis | Test | Case ( | Sensitivity (%) | Specificity (%) | Accuracy (%) |
|---|---|---|---|---|---|
| Cytology analysis | 56 | 65 | 93.8 | 73.2 | |
| Pancreatic cancer | Cytology analysis + MUC1(+) | 56 | 85 | 100 | 89.3 |
| Cytology analysis + MUC5AC(+) | 56 | 90 | 93.8 | 91.1 |
Studies of molecular biologic diagnosis of pancreatic carcinoma using specimens obtained by EUS-FNA.
|
Biological analyses | Author | Year | EUS-FNA samples | Sensitivity | Specificity | Positive predictive value | Negative positive value | Accuracy | Diagnosis |
|---|---|---|---|---|---|---|---|---|---|
|
Reicher et al. [ | 2011 | 46 | 87.9% | 93.8% | 96.7% | 78.9% | 89.8% | Combination with cytology and FISH | |
| KRAS | Bournet et al. [ | 2009 | 178 | 88.0% | 100% | 100% | 63.0% | 90.0% | Combination with cytopathology |
| Maluf-Filho et al. [ | 2007 | 74 | 90.9% | 47.6% | 89.5% | 98.1% | 89.2% | Combination with cytopathology | |
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| P53 | Jahng et al. [ | 2010 | 61 | 51.0% | 100% | Combination with cytology | |||
| Itoi et al. [ | 2005 | 62 | 90.0% | 91.0% | 92% | Combination with cytopathology | |||
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| P16 | Salek et al. [ | 2007 | 101 | 85.0% | 100.0% | Monitoring the loss of heterozygosity | |||
| SMAD4 | Salek et al. [ | 2007 | 101 | 78.0% | 57.0% | Monitoring the loss of heterozygosity | |||
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| MUCs | Wang et al. [ | 2007 | 40 | 100% | 91.1% | MUC5AC+cytology | |||
| Giorgadze et al. [ | 2006 | 30 | 70% | 100% | 100% | 100% | 75% | Combination of MUC1+/ MUC2−/ MUC5AC+ | |
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| S100P | Kosarac et al. [ | 2011 | 14 | 78.2% | 87.5% | ||||
| Daniel et al. [ | 2011 | 62 | 90.0% | 67.0% | |||||
*FISH: fluorescense in situ hybridization.