| Literature DB >> 17645803 |
Vera L Costa1, Rui Henrique, Franclim R Ribeiro, Mafalda Pinto, Jorge Oliveira, Francisco Lobo, Manuel R Teixeira, Carmen Jerónimo.
Abstract
BACKGROUND: Aberrant promoter hypermethylation of cancer-associated genes occurs frequently during carcinogenesis and may serve as a cancer biomarker. In this study we aimed at defining a quantitative gene promoter methylation panel that might identify the most prevalent types of renal cell tumors.Entities:
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Year: 2007 PMID: 17645803 PMCID: PMC1940017 DOI: 10.1186/1471-2407-7-133
Source DB: PubMed Journal: BMC Cancer ISSN: 1471-2407 Impact factor: 4.430
Clinical and pathological characteristics of patient population
| Clinicopathological feature | |
| Patients, n | 85 |
| Gender, n (%) | |
| Male | 52 (61.2) |
| Female | 33 (38.8) |
| Age, yr, median (range) | 61 (36–86) |
| Histologic subtype, n (%) | |
| Clear cell RCC | 52 (61.2) |
| Papillary RCC | 13 (15.2) |
| Chromophobe RCC | 10 (11.8) |
| Oncocytoma | 10 (11.8) |
| Pathologic stage*, n (%) | |
| T1 | 42 (56) |
| T2 | 15 (20) |
| T3 | 16 (21.4) |
| T4 | 2 (2.6) |
| Furhman grade, n (%) | |
| 1 | 2 (2.7) |
| 2 | 24 (32.0) |
| 3 | 36 (48.0) |
| 4 | 13 (17.3) |
RCC, renal cell carcinoma, * only includes RCC cases
Percentage and frequency of methylation [% (n)] of cancer-related genes in subtypes of renal cell carcinoma (RCC), oncocytoma, and morphologically normal renal tissue (NRT)
| Clear cell RCC | Papillary RCC | Chromophobe RCC | Oncocytoma | NRT | ||
| % (n = 52) | % (n = 13) | % (n = 10) | % (n = 10) | % (n = 62) | ||
| 5q21-q22 | 19.2 (10) | 23.1 (3) | 0 (0) | 0 (0) | 8.1 (5) | |
| 1p31 | 100 (52) | 100 (13) | 100 (10) | 100 (10) | 100 (62) | |
| 16q22.1 | 82.7 (43) | 69.2 (9) | 20 (2) | 30 (3) | 87.1 (54) | |
| 3p21 | 0 (0) | 0 (0) | 0 (0) | 0 (0) | 0 (0) | |
| 22q12.3 | 100 (52) | 100 (13) | 100 (10) | 100 (10) | 100 (62) | |
| 9p21 | 9.6 (5) | 7.7 (1) | 10 (1) | 20 (2) | 27.4 (17) | |
| 9p21 | 0 (0) | 0 (0) | 0 (0) | 0 (0) | 0 (0) | |
| 3p21.3 | 80.8 (42) | 100 (13) | 40 (4) | 90 (9) | 100 (62) | |
| 11q13 | 5.8 (3) | 15.4 (2) | 0 (0) | 0 (0) | 0 (0) | |
| 7q21.1 | 86.5 (45) | 84.6 (11) | 80 (8) | 90 (9) | 96.8 (60) | |
| 1p36.3 | 100 (52) | 100 (13) | 100 (10) | 100 (10) | 100 (62) | |
| 1q25.2-q25.3 | 96.1 (50) | 92.3 (12) | 90 (9) | 90 (9) | 100 (62) | |
| 1p36.11 | 19.2 (10) | 23.1 (3) | 0 (0) | 0 (0) | 24.2 (15) | |
| 6q25.1 | 67.3 (35) | 76.9 (10) | 60 (6) | 80 (8) | 77.4 (48) | |
| 14q23.2 | 55.8 (29) | 46.1 (6) | 50 (5) | 30 (3) | 43.5 (27) | |
| 3p14.2 | 51.9 (27) | 53.8 (7) | 50 (5) | 50 (5) | 69.3 (43) | |
| 10q26 | 1.9 (1) | 0 (0) | 0 (0) | 0 (0) | 11.3 (7) | |
| 3p24 | 1.9 (1) | 0 (0) | 0 (0) | 0 (0) | 0 (0) |
Distribution of methylation levels of cancer-related genes in subtypes of renal cell carcinoma (RCC), oncocytoma, and morphologically normal renal tissue (NRT) [(target gene/ACTB) × 1000 expressed as median (interquartile range)]
| Clear cell RCC | Papillary RCC | Chromophobe RCC | Oncocytoma | NRT | ||
| 0 (0-0) | 0 (0-0) | 0 (0-0) | 0 (0-0) | ns | 0 (0-0) | |
| 942.6 (634.7–1746.6) | 807.2 (623.3–1322.6) | 198.6 (148.7–1575.5) | 930.1 (641.5–1654.5) | ns | 893.5 (574.2–1286.2) | |
| 3.8 (0.5–12.3) | 3.5 (0–19.3) | 0 (0-0) | 0 (0–1.1) | 0.0007 | 2.3 (0.52–6.72) | |
| 0 (0-0) | 0 (0-0) | 0 (0-0) | 0 (0-0) | ns | 0 (0-0) | |
| 1441.4 (947.3–2592.1) | 1048.2 (848.3–1354.5) | 1192.4 (687.9–1477.4) | 1302.5 (738.6–2591.6) | ns | 1088.4 (790.2–1497.1) | |
| 0 (0-0) | 0 (0-0) | 0 (0-0) | 0 (0-0) | ns | 0 (0–0.04) | |
| 0 (0-0) | 0 (0-0) | 0 (0-0) | 0 (0-0) | ns | 0 (0-0) | |
| 71.7 (4.7–265.5) | 433.2 (236.4–966.0) | 0 (0–2.7) | 10.6 (2.2–27.5) | 0.0001 | 59.6 (33.1–88.5) | |
| 0 (0-0) | 0 (0-0) | 0 (0-0) | 0 (0-0) | ns | 0 (0-0) | |
| 25.3 (10.5–58.2) | 15.5 (6.0–23.7) | 33.1 (2.6–54.9) | 33.5 (7.9–117.9) | ns | 31.6 (16.6–41.9) | |
| 556.4 (236.9–965.9) | 349.0 (181.6–561.9) | 572.8 (340.3–887.0) | 667.5 (634.4–1687.9) | ns | 419.7 (305.2–614.3) | |
| 72.9 (34.1–222.5) | 17.7 (9.3–43.2) | 6.0 (3.9–49.7) | 16.2 (5.3–28.9) | 0.002 | 54.6 (34.4–90.8) | |
| 0 (0-0) | 0 (0-0) | 0 (0-0) | 0 (0-0) | ns | 0 (0-0) | |
| 6.9 (0–31.3) | 4.4 (2–10.9) | 3.8 (0–19.1) | 12.9 (7.7–76.5) | ns | 15.0 (0.9–35.5) | |
| 0.6 (0–1.9) | 0 (0–0.4) | 0.3 (0–2.7) | 0 (0–0.5) | ns | 0 (0–0.3) | |
| 0.7 (0–5.6) | 2.6 (0–47.0) | 0.9 (0–4.0) | 0.4 (0–6.6) | ns | 2.0 (0–17.7) | |
| 0 (0-0) | 0 (0-0) | 0 (0-0) | 0 (0-0) | ns | 0 (0-0) | |
| 0 (0-0) | 0 (0-0) | 0 (0-0) | 0 (0-0) | ns | 0 (0-0) |
*Kruskall-Wallis one-way analysis of variance test among the four groups of renal cell tumors; IQR, interquartile range; ns, not significant
Figure 1Methylation levels. Distribution of promoter methylation levels [(target gene/ACTB) × 1000] of (A) CDH1, (B) PTGS2, and (C) RASSF1A in clear cell (ccRCC), papillary (pRCC), and chromophobe (chRCC) renal carcinomas, and oncocytomas.
Validity estimates of CDH1, PTGS2, and RASSF1A hypermethylation for discrimination among subtypes of renal cell tumor
| ccRCC & pRCC | 61.3% | 91.3% | 95.0% | 46.7% | |
| ccRCC | 46.2% | 90.9% | 88.9% | 51.7% | |
| pRCC | 76.9% | 75.0% | 35.7% | 94.7% |
ccRCC, clear cell renal cell carcinoma; chRCC, chromophobe renal cell carcinoma; pRCC, papillary renal cell carcinoma; PPV, positive predictive value; NPV, negative predictive value