| Literature DB >> 16495917 |
A L Oei1, L F Massuger, J Bulten, M J Ligtenberg, N Hoogerbrugge, J A de Hullu.
Abstract
To determine the effectiveness of annual gynaecological screening (pelvic examination, transvaginal ultrasound, and CA-125), a prospective cohort study of women at high risk for hereditary ovarian cancer was conducted. Women were offered DNA analysis followed by either annual screening or prophylactic bilateral salpingo-oophorectomy (BSO). Study population consisted of 512 high-risk women (median follow-up 2.07 years, range 0-9.4 years): 265 women (52%) had a BRCA mutation. Persisting abnormalities indicated diagnostic surgery in 24 women resulting in one primary ovarian cancer FIGO stage IIIc was found. The effectiveness of screening was studied by calculating the probability of finding ovarian cancers in the BRCA-1 and BRCA-2 carrier group and comparing this to the identified number of ovarian cancers. The number of ovarian cancer patients found at surveillance was in accordance with the predicted number of ovarian cancers. A total number of 169 women underwent prophylactic BSO: one ovarian cancer stage IIb was found. In conclusion, the surveillance programme for hereditary ovarian cancer does identify patients with ovarian cancer but is very inefficient considering the high number of surveillance visits and the advanced stage of ovarian cancer in the identified patient. For prevention of advanced stage ovarian cancer, prophylactic BSO from age 35-40 years is a more efficient alternative.Entities:
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Year: 2006 PMID: 16495917 PMCID: PMC2361371 DOI: 10.1038/sj.bjc.6603015
Source DB: PubMed Journal: Br J Cancer ISSN: 0007-0920 Impact factor: 7.640
Criteria for referral to the gynaecologist for ovarian surveillance (Vasen ; Sutcliffe )
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| • | Women with a proven |
| • | Women from a family with a proven |
| • | Women with first- or second-degree relatives with breast cancer before the age of 50, and ovarian cancer in the family. |
| • | Two first-degree relatives or one first-degree and one second-degree relative with ovarian cancer, independent of age. |
Patient characteristics of 512 women at primary surveillance
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| Median age | 42 years | Range 20–75 years |
| Median follow-up | 2.07 years | Range 0–9.4 years |
| Type mutation no. (%) | Number | Percentage |
| | 180 | (34.2%) |
| | 84 | (16%) |
| | 1 | (0.2%) |
| No mutation | 99 | (19.1%) |
| Unknown | 6 | (1.5%) |
| Not tested | 142 | (27.3%) |
| Menopausal state | 502 | |
| Pre-menopausal | 372 | (72.7%) |
| Post-menopausal | 130 | (25.4%) |
| Missing | 10 | (1.9%) |
| Previous oral contraceptive use | 199 | (38.8%) |
| Previous pregnancy | 403 | (78.7%) |
| Previous breast cancer | 165 | (32.1%) |
| Previous abdominal surgery | 171 | (33.4%) |
| Unknown | 10 | (1.9%) |
These patients underwent DNA testing during the surveillance programme and appeared to have no mutation.
Abdominal surgery: for example, caesarean section(s), abdominal hysterectomy, salpingo-oophorectomy and appendectomy or other abdominal operations.
Overview of initially abnormal findings at surveillance and follow-up
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| Pelvic examination ( | 11 (2%) | 5 (45%) |
| CA-125 (U ml−1) ( | 50 (4%) | 43 (86%) |
| Transvaginal ultrasound ( | 317 (21%) | 295 (93%) |
| Total ( | 378 (9 %) |
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91% in bold emphasizes the percentage.
Overview of indications and results of diagnostic laparoscopies in 24 women
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| Abnormal pelvic examination | 0 | 0 |
| Abnormal CA-125 (⩾35 U ml−1) | 1 | 1 – No abnormalities |
| Abnormal ultrasound | 12 | 8 – Ovarian benign tumour |
| 3 – No abnormalities | ||
| 1 – Haemorrhagic corpus luteum | ||
| Abnormal pelvic examination and CA-125 (⩾35 U ml−1) | 1 | 1 – No abnormalities |
| Abnormal pelvic examination and ultrasound | 4 | 4 – Ovarian benign tumour |
| Abnormal CA-125 (⩾35 U ml−1) and ultrasound | 5 | 1 – Salpingitis and paratubal cyst |
| 1 – Metastasis of breast cancer | ||
| 1 – No abnormalities | ||
| 1 – Endometriosis | ||
| Abnormal pelvic examination, CA-125 (⩾35 U ml−1) and ultrasound | 1 | 1 – Metastasis of breast cancer |
FIGO, International Federation of Gynecology and Obstetrics.
In this group two patients had diagnostic laparoscopy converted to laparotomy.
In this group one patient had diagnostic laparoscopy converted to laparotomy.
Ovarian cancer FIGO IIIc in bold emphasizes the finding of only one ovarian cancer.
BRCA-1 mutation carriers incidence during surveillance
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| 20–24 | 4.37 | 0.76 | 0.001 | 0.001 | 0.004 | 0.001 | 9 | 6 |
| 25–29 | 38.54 | 2.65 | 0.002 | 0.002 | 0.077 | 0.005 | 69 | 10 |
| 30–34 | 80.05 | 30.16 | 0.18 | 0.004 | 14.409 | 0.120 | 115 | 43 |
| 35–39 | 75.61 | 20.06 | 0.28 | 0.01 | 21.170 | 0.200 | 158 | 34 |
| 40–44 | 25.51 | 6.45 | 0.87 | 0.08 | 22.193 | 0.516 | 53 | 18 |
| 45–49 | 12.15 | 12.79 | 1.49 | 0.14 | 18.103 | 1.790 | 26 | 29 |
| 50–54 | 5.12 | 4.38 | 0.96 | 0.6 | 4.915 | 2.628 | 19 | 12 |
| 55–59 | 3.54 | 3.60 | 1.19 | 0.75 | 4.212 | 2.700 | 13 | 12 |
| 60–64 | 0.80 | 1.53 | 2.26 | 0.38 | 1.808 | 0.581 | 3 | 5 |
| 65–69 | 2.09 | 0.30 | 2.49 | 0.42 | 5.204 | 0.126 | 4 | 1 |
| >70 | 0.30 | 0.001 | 1 | |||||
| Total | 248.1 | 82.68 | 92.095 | 8.667 | 470 | 170 | ||
Based on incidence rates of Antoniou et al (2003).
Overview of literature: surveillance for ovarian cancer in high-risk women
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| Mean age of patients in years (range) | 40 (20–75) | Unknown | 42 (18–77) | Unknown | 47 (22–70) | 47.7 (24.1–79) | 45.5 (35–77.7) | 41 (18–77) |
| No. of patients | 512 high-risk women | 1110 high-risk women | 383 high-risk women | 138 high-risk women | 311 high-risk women | 251 mutation carriers | 170 mutation carriers | 754 high-risk women |
| No. of patients with a mutation | 180 | Unknown | 127 | 77 | 26 | 251 (distribution unknown) | 104 | Not tested |
| 84 | 25 | 18 | 5 | 66 | ||||
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| No. of surveillance consults | 1621 | 3701 | 1273 | 227 | 1555 | Unknown (89 women) | 350 | Unknown |
| No. of diagnostic surgeries | 24 | 29 | 20 | 36 | 9 | 10 | 11 | Unknown |
| Incidence of cancer in women undergoing surveillance (FIGO stage) | 1 ovarian | 10 ovarian | 1 × breast metastasis | 6 ovarian | 1 ovarian | 4 ovarian | 4 ovarian | 16 ovarian |
| 1 × Stage IIIc | 3 × Stage Ic | 5 × stage III | Stage Ia | 2 × Stage 1 | 1 peritoneal | 06 × Stage I | ||
| 1 × Stage Iib | 1 × stage IV | 1 × Stage II | 4 × Borderline stage I Others unknown | |||||
| 1 × Stage Iic | 1 × Unstaged | |||||||
| 1 × Stage IIIb | 1 peritoneal | |||||||
| 3 × Stage IIIc | ||||||||
| 1 × Stage IV | ||||||||
| Incidence of interval cancers | 0 | 2 | 2 | 0 | 0 | 0 | 0 | 0 |
| No of patients choosing for prophylactic BSO | 169 | Unknown | 133 | 97 | Not performed | 90 | 98 | Not performed |
| Incidence of diagnosed cancers at prophylactic BSO | 1 ovarian | 1 ovarian | 1 fallopian | 1 ovarian | Not applicable | 2 ovarian | 1 peritoneal | Not applicable |
| 1 × Stage IIb | 1 × Stage IIIa | tube | Stage Iic | 2 × Stage I | ||||
| 2 breast metastasis | Stage Ia | 2 fallopian | ||||||
| 1 breast | tube | |||||||
| metastasis | 1 × Stage I | |||||||
| 1 × Stage II |
Note: All stages ordered in FIGO stage, International Federation of Gynecology and Obstetrics.