| Literature DB >> 17311016 |
E Bågeman1, C Ingvar, C Rose, H Jernström.
Abstract
Multiparity decreases the risk of breast cancer in white women, whereas it is a risk factor in black women <50 years. Early-onset breast cancer (<50 years) has been associated with high insulin-like growth factor-1 (IGF-1) levels. Absence of the common IGF1 19 cytosine-adenine (CA)-repeat allele (IGF1-19/-19) inverts the effect of several non-genetic factors on breast cancer risk but the interaction between IGF1-19/-19 and multiparity on breast cancer risk is unknown. As IGF1-19/-19, multiparity and early-onset breast cancer are more common in black than in white women, we aimed to study whether multiparity combined with IGF1-19/-19 increases the risk of early-onset breast cancer. Four hundred and three breast cancer patients diagnosed in Lund, Sweden, at age 25-99 years were genotyped for the IGF1 CA-repeat length using fragment analysis. Overall, 12.9% carried the IGF1-19/-19 genotype. There was a highly significant interaction between multiparity and IGF1-19/-19 on age at breast cancer diagnosis (P=0.007). Among IGF1-19/-19 patients, multiparity was associated with a 9.2 year earlier age at diagnosis compared with uniparity or nulliparity (P=0.006). Multiparity combined with IGF1-19/-19 was associated with an early age at breast cancer diagnosis. If confirmed, IGF1-19/-19 may help identify a subgroup of women for earlier breast cancer screening.Entities:
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Year: 2007 PMID: 17311016 PMCID: PMC2360065 DOI: 10.1038/sj.bjc.6603632
Source DB: PubMed Journal: Br J Cancer ISSN: 0007-0920 Impact factor: 7.640
Baseline characteristics of all patients, patients younger than 50 years and patients aged 50 years or older
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| Age at diagnosis (years) | 58.5 (11.5) | 403/403 | 43.4 (5.2) | 96/96 | 63.2 (8.4) | 307/307 |
| Age at menarche (years) | 13.25 (1.3) | 399/403 | 12.9 (1.2) | 94/96 | 13.4 (1.3) | 305/307 |
| Pre-menopausal (%) | 25 | 402/403 | 75 | 96/96 | 9 | 306/307 |
| Age at menopause (years) | 49.1 (5.1) | 290/403 | 39.7 (5.8) | 17/96 | 49.7 (4.4) | 273/307 |
| Pregnancies | 2.3 (1.4) | 403/403 | 2.5 (1.4) | 96/96 | 2.2 (1.4) | 307/307 |
| Parity | 1.9 (1.2) | 403/403 | 1.8 (1.0) | 96/96 | 1.9 (1.2) | 307/307 |
| Age at first full-term pregnancy, in parous women | 25.1 (4.9) | 334/403 | 26.6 (4.3) | 82/96 | 24.6 (4.9) | 252/307 |
| OC | 69 | 403/403 | 91 | 96/96 | 62 | 307/307 |
| HRT, ever | 45 | 403/403 | 11 | 96/96 | 56 | 307/307 |
| Current smoker, yes | 22 | 403/403 | 18 | 96/96 | 23 | 307/307 |
| Current teetotaller, yes | 11 | 403/403 | 13 | 96/96 | 11 | 307/307 |
| 1 and/or 2° relative with breast cancer | 34 | 388/403 | 37 | 92/96 | 33 | 296/307 |
| BMI (kg/m2) | 25.3 (4.4) | 401/403 | 24.3 (4.4) | 96/96 | 25.6 (4.3) | 305/307 |
| Waist to hip ratio | 0.84 (0.08) | 399/403 | 0.82 (0.08) | 94/96 | 0.84 (0.08) | 305/307 |
| Total breast volume (cm3) | 1156 (682) | 394/403 | 985 (574) | 93/96 | 1208 (705) | 301/307 |
Abbreviations: BMI, body mass index; HRT, hormone replacement therapy; OC, oral contraceptives.
The allele frequencies of the IGF1 CA-repeat allele in all patients. The percentage does not add up to 100%, because it was rounded off
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| 11 | 1 | (0.1) |
| 12 | — | |
| 13 | — | |
| 14 | — | |
| 15 | 1 | (0.1) |
| 16 | — | |
| 17 | 21 | (2.6) |
| 18 | 31 | (3.8) |
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| ( |
| 20 | 167 | (20.7) |
| 21 | 46 | (5.7) |
| 22 | 12 | (1.5) |
| 23 | 2 | (0.2) |
Abbreviations: CA, cytosine-adenine; IGF, insulin-like growth factor.
This is the most common repeat length.
The common 19 repeat allele is bolded.
Figure 1Frequency of the IGF1-19/-19 genotype in the 403 patients according to age at diagnosis. The total number of women in each age category is indicated. The IGF1-19/-19 genotype was most common (over 20 %) in patients diagnosed before age 45 years and in patients diagnosed between the ages of 55 and 59 years and thus displayed a biphasic distribution.
Age (mean,±s.d.) at breast cancer diagnosis in relation to multiparity and IGF1 genotype
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| 0–1 children | 58.0 (±12.1) | 62.3 (±10.9) | |
| 2+ children | 59.3 (±11.3) | 53.1 (±9.5) | |
Abbreviations: CA, cytosine-adenine; IGF, insulin-like growth factor. There was a significant interaction on age at breast cancer diagnosis in multiparous patients and in patients having less then two children depending on the presence (IGF1+19) or absence (IGF1-19/-19) of the IGF1 19 CA-repeat allele