Possible Role of Ovarian Epithelial Inflammation in Ovarian Cancer

Ness, Roberta B.; Cottreau, Carrie

doi:10.1093/jnci/91.17.1459

Cited by 509 publications

(357 citation statements)

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“…Early menarche is associated with a more rapid onset of ovulatory cycles, and with the tendency to sustain higher levels of luteal phase estradiol and progesterone (Vihko and Apter, 1984). Thus, a protective effect of late menarche, observed here in premenopausal women, is consistent with hypotheses regarding incessant ovulation (Fathalla, 1971;Casagrande et al, 1979) and ovarian inflammation (Ness and Cottreau, 1999), but inconsistent with the hypothesis that higher levels of progesterone are associated with reduced risk (Risch, 1998). Similar to most previous reports (for example, Hartge et al, 1988;Chen et al, 1992), we found no evidence of an association between age at natural menopause and ovarian cancer risk.…”

Section: Discussionsupporting

confidence: 87%

“…The gonadotrophin hypothesis proposes that excessive gonadotropin secretion and consequent increases in oestrogen stimulation lead to proliferation and malignant transformation of ovarian epithelium . More recent hypotheses have suggested a role for chronic ovarian inflammation (Ness, 1999), androgens and progesterone (Risch, 1998), and the possibility that pregnancies reduce risk by clearing transforming cells from the ovaries (ovarian clearance) (Adami et al, 1994). …”

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confidence: 99%

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Menstrual and reproductive factors in relation to ovarian cancer risk

et al. 2001

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The reduced risk of epithelial ovarian cancer associated with parity and oral contraceptive use suggests that pituitary and/or ovarian hormones or ovulatory events are important in the aetiology of these tumours (Cramer, 1986). Nevertheless, despite extensive study, the influence of menstrual and reproductive factors, with the exception of parity, remains uncertain. In this report, we evaluate menstrual and reproductive characteristics in relation to ovarian cancer risk overall, and in relation to the major tumour histologic subtypes. Our findings are considered in light of several current hypotheses regarding ovarian cancer pathogenesis. Briefly, the incessant ovulation hypothesis suggests that risk is increased by chronic post-ovulatory trauma to the epithelial surface of the ovary, and the tendency to form inclusion cysts (Fathalla, 1971;Casagrande et al, 1979). The gonadotrophin hypothesis proposes that excessive gonadotropin secretion and consequent increases in oestrogen stimulation lead to proliferation and malignant transformation of ovarian epithelium . More recent hypotheses have suggested a role for chronic ovarian inflammation (Ness, 1999), androgens and progesterone (Risch, 1998), and the possibility that pregnancies reduce risk by clearing transforming cells from the ovaries (ovarian clearance) (Adami et al, 1994). METHODSWe conducted a population-based, case-control study of epithelial ovarian cancer in eastern Massachusetts (MA) and New Hampshire (NH). The methods used have been previously described Harlow et al, 1998). Briefly, 1033 potentially eligible case women (ages 20 to 74) were ascertained between May 1992 and March 1997 through state-wide cancer registries (NH, MA) and hospital tumour boards (MA). After exclusion of patients who had nonepithelial tumours (n = 52), and those who had died (n = 91), moved out of state (n = 27), had no telephone (n = 24), or did not speak English (n = 14), 825 case women were eligible for the study. Physicians denied permission to contact 126 (14%) of these women, and 136 (16%) of women declined to participate. This analysis is based on 563 cases of epithelial ovarian cancer, including lesions of borderline malignancy.Control women were identified primarily by random digit dialing (RDD) (Waksberg, 1978), and matched to case women by age (within 4 years) and telephone sampling unit. Of approximately 5400 residential households contacted, 10% declined to provide a household census, and 80% provided a census, but lacked a potentially eligible control subject. In the remaining 10% of households, a potentially eligible control was identified. 72% of the potential control women agreed to participate in the study. In MA, control women of age 60 or older were randomly chosen from Town Books, and matched to case women by age and precinct. Of 328 control women selected from Town Books, 21% Summary We assessed menstrual and reproductive factors in relation to ovarian cancer risk in a large, population-based, case-control study. 563 cases in Massachusetts and New Hampsh...

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Section: Discussionsupporting

confidence: 87%

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confidence: 99%

Menstrual and reproductive factors in relation to ovarian cancer risk

et al. 2001

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“…26 In addition, normal ovarian epithelial cells themselves have been previously reported to produce several proinflammatory cytokines, such as monocyte colony-stimulating factor (M-CSF), IL-1, IL-6 and TNF-␣ in response to injury or inflammatory stimuli. 27,28 On the basis of epidemiologic studies, it has been proposed that chronic inflammation may play a role in the development of ovarian tumors, 29 and IL-18 has been considered an important mediator of chronic inflammation in other areas. 30 In keeping with previous reports of IL-18 expression in epithelial layers that line the mucosal surface of the body, we report for the first time that normal ovarian epithelial cells express both IL-18 and ICE and have the potential to produce mature IL-18.…”

Section: Discussionmentioning

confidence: 99%

Expression of interleukin‐18 in human ovarian carcinoma and normal ovarian epithelium: Evidence for defective processing in tumor cells

Wang

Gaggero

Rubartelli

et al. 2002

Intl Journal of Cancer

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“…Repeated episodes of ovulation-associated injury and repair are presumed to underlie the high frequency of ovarian carcinoma arising from the OSE (Fathalla, 1971;Salazar et al, 1996), which account for 90% of all ovarian cancers (Ozols, 1991). Since ovulation is a natural inflammatory process (Espey, 1980a, b), factors related to inflammation of the OSE have been associated with increased risk of ovarian cancer (Ness and Cottreau, 1999;Ness et al, 2000). It is therefore critically important to understand how inflammatory cell damage is normally resolved in the OSE.…”

mentioning

confidence: 99%

“…Mutations responsible for generating cancerous cells are believed to arise from DNA replication/repair errors during subsequent rounds of OSE cell proliferation. The rate of mutation is further believed to increase in the presence of toxic oxidants that are released during such an inflammatory response (Ness and Cottreau, 1999).…”

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confidence: 99%

Inflammation-associated gene expression is altered between normal human ovarian surface epithelial cells and cell lines derived from ovarian adenocarcinomas

et al. 2005

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Ovulation is believed to contribute to the development of ovarian cancers that derive from the ovarian surface epithelium (OSE). The process of ovulation is synonymous with inflammation and inflammatory cytokines such as interleukin-1a (IL-1a) have recently been shown to induce both inflammatory and anti-inflammatory responses in human OSE (HOSE) cells. In this study we directly compared levels of IL-1a-induced gene expression by analysing the levels of 11b-hydroxysteroid dehydrogenase (11bHSD) types 1 (11bHSD-1) and 2 (11bHSD-2), cyclooxygenase-2 (COX-2), IL-1 receptor (IL-1R) and glucocorticoid receptor a (GRa) mRNA between normal HOSE cells and cell lines derived from poorly differentiated (SKOV-3, BG-1, PEO-4) and well-differentiated (PEO-14) ovarian adenocarcinoma. In HOSE cell cultures, and to a lesser extent PEO-14 cells, the basal mRNA levels of COX-2 and 11bHSD-1 were relatively high and further shown to be induced in response to IL-1a (for HOSE cells; 420-fold, Po0.05 and PEO-14 cells; 43fold, Po0.05). However, whereas HOSE cells expressed a low level of 11bHSD-2 mRNA that was only mildly responsive to IL-1a (1.3-fold, Po0.001), all cell lines exhibited a higher basal level of 11bHSD-2 mRNA that was in some cases further stimulated in PEO-4 cells (five-fold; Po0.05) or suppressed in SKOV-3 cells (two-fold; Po0.01) in response to IL-1a. All cells tested expressed IL-1R and, with the exception of BG-1, GRa. These results indicate that cell lines derived from ovarian cancers have lost the ability to respond normally to inflammatory cytokines such as IL-1a. The finding that normal OSE cells, in contrast to cell lines derived from patients with ovarian adenocarcinoma, abundantly express 11bHSD-1 mRNA but are essentially devoid of 11bHSD-2 mRNA supports the concept that the pattern of 11bHSD isoform gene expression is a defining feature of neoplastic cellular transformation, which might have particular relevance to the ovary.

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Possible Role of Ovarian Epithelial Inflammation in Ovarian Cancer

Cited by 509 publications

References 103 publications

Menstrual and reproductive factors in relation to ovarian cancer risk

Menstrual and reproductive factors in relation to ovarian cancer risk

Expression of interleukin‐18 in human ovarian carcinoma and normal ovarian epithelium: Evidence for defective processing in tumor cells

Inflammation-associated gene expression is altered between normal human ovarian surface epithelial cells and cell lines derived from ovarian adenocarcinomas

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