Jump to content

Endometrial hyperplasia

From Wikipedia, the free encyclopedia
Endometrial hyperplasia
Micrograph showing simple endometrial hyperplasia, where the gland-to-stroma ratio is preserved but the glands have an irregular shape and/or are dilated. Endometrial biopsy. H&E stain.
SpecialtyGynaecology Edit this on Wikidata

Endometrial hyperplasia is a condition of excessive proliferation of the cells of the endometrium, or inner lining of the uterus.

Most cases of endometrial hyperplasia result from high levels of estrogens, combined with insufficient levels of the progesterone-like hormones which ordinarily counteract estrogen's proliferative effects on this tissue. This may occur in a number of settings, including obesity, polycystic ovary syndrome, estrogen producing tumours (e.g. granulosa cell tumour) and certain formulations of estrogen replacement therapy.

Endometrial hyperplasia with atypia is a significant risk factor for the development or even co-existence of endometrial cancer, so careful monitoring and treatment of women with this disorder is essential.

Classification

[edit]
Histopathology of complex hyperplasia without atypia: Cystically dilated endometrial glands lined by a single layer of columnar epithelium.[1]
Histopathology of complex hyperplasia with atypia: Closely packed endometrial glands with sparse intervening stroma and stratification of the lining epithelium. Epithelial cells show cytological atypia with high nucleocytoplasmic ratio, irregular clumping of nuclear chromatin, and mitotic figures.[2]

Like other hyperplastic disorders, endometrial hyperplasia initially represents a physiological response of endometrial tissue to the growth-promoting actions of estrogen. However, the gland-forming cells of a hyperplastic endometrium may also undergo changes over time which predispose them to cancerous transformation. Several histopathology subtypes of endometrial hyperplasia are recognisable to the pathologist, with different therapeutic and prognostic implications.[3]

The most commonly used classification system for endometrial hyperplasia is the World Health Organization (WHO) system, which previously had four categories: simple hyperplasia without atypia, complex hyperplasia without atypia, simple atypical hyperplasia and complex atypical hyperplasia.[4] In 2014, the WHO updated the classification system and removed the distinction between simple or complex hyperplasia, instead only on presence or absence of atypia.[5]

  • Endometrial hyperplasia (simple or complex) - Irregularity and cystic expansion of glands (simple) or crowding and budding of glands (complex) without worrisome changes in the appearance of individual gland cells. In one study, 1.6% of patients diagnosed with these abnormalities eventually developed endometrial cancer.[6]
  • Atypical endometrial hyperplasia (simple or complex) - Simple or complex architectural changes, with worrisome (atypical) changes in gland cells, including cell stratification, tufting, loss of nuclear polarity, enlarged nuclei, and an increase in mitotic activity. These changes are similar to those seen in true cancer cells, but atypical hyperplasia does not show invasion into the connective tissues, the defining characteristic of cancer. The previously mentioned study found that 22% of patients with atypical hyperplasia eventually developed cancer.[6]

Diagnosis

[edit]

Diagnosis of endometrial hyperplasia can be made by endometrial biopsy, which is done in the office setting or through curettage of the uterine cavity to obtain endometrial tissue for histopathologic analysis. A workup for endometrial disease may be prompted by abnormal uterine bleeding, or the presence of atypical glandular cells on a pap smear.[7]

Prognosis

[edit]

Many studies have shown that endometrial hyperplasia can progress to cancer, particularly when there are atypical cells. Nevertheless, such studies has typically dealt with atypical hyperplasia. A review of 65 articles on estimated risk of progression to cancer concludes that none of those studies reported estimates specifically for non-atypical hyperplasia patients. Further it states the need for population based studies including both non-atypical and atypical hyperplasia to accurately estimate the risk of progression to cancer.[8]

If untreated with hysterectomy, endometrial hyperplasia progresses to adenocarcinoma within 20 years in:

  • 28% of cases with atypia (95% CI, 8.6% to 42.5%), and
  • about 5% of cases without atypia.[9]

The rates are more favorable in cases with simple rather than complex hyperplasia,[10] but as mentioned above this terminology was phased out of the WHO classification in 2014.

In patients with samples showing atypia, carcinoma is already present in over 40% of cases.[11][12] Given this, the aforementioned 28% atypia progression rate may be an underestimate, and the true number may closer to the 42.5% part of the study's remarkably wide confidence interval.

Treatment

[edit]

Treatment of endometrial hyperplasia is individualized, and may include hormonal therapy, such as cyclic or continuous progestin therapy, or hysterectomy.[7]

See also

[edit]

References

[edit]
  1. ^ Rao, Shalinee; Sundaram, Sandhya; Narasimhan, Raghavan (2009). "Biological behavior of preneoplastic conditions of the endometrium: A retrospective 16-year study in south India". Indian Journal of Medical and Paediatric Oncology. 30 (4): 131–135. doi:10.4103/0971-5851.65335. ISSN 0971-5851. PMC 2930300. PMID 20838554.
    - Figure- available via license: Creative Commons Attribution 2.0 Generic
  2. ^ Rao, Shalinee; Sundaram, Sandhya; Narasimhan, Raghavan (2009). "Biological behavior of preneoplastic conditions of the endometrium: A retrospective 16-year study in south India". Indian Journal of Medical and Paediatric Oncology. 30 (4): 131–135. doi:10.4103/0971-5851.65335. ISSN 0971-5851. PMC 2930300. PMID 20838554.
    - Figure- available via license: Creative Commons Attribution 2.0 Generic
  3. ^ Cote, Richard; Suster, Saul; Weiss, Lawrence; et al., eds. (2002). Modern Surgical Pathology (2 Volume Set). London: W B Saunders. ISBN 0-7216-7253-1.[page needed]
  4. ^ Skov, B. G.; Broholm, H; Engel, U; Franzmann, M. B.; Nielsen, A. L.; Lauritzen, A. F.; Skov, T (1997). "Comparison of the reproducibility of the WHO classifications of 1975 and 1994 of endometrial hyperplasia". International Journal of Gynecological Pathology. 16 (1): 33–7. doi:10.1097/00004347-199701000-00006. PMID 8986530. S2CID 26446736.
  5. ^ Emons, G.; Beckmann, M. W.; Schmidt, D.; Mallmann, P. (February 2015). "New WHO Classification of Endometrial Hyperplasias". Geburtshilfe und Frauenheilkunde. 75 (2): 135–136. doi:10.1055/s-0034-1396256. ISSN 0016-5751. PMC 4361167. PMID 25797956.
  6. ^ a b Kurman, Robert J.; Kaminski, Paul F.; Norris, Henry J. (1985). "The behavior of endometrial hyperplasia. A long-term study of "untreated" hyperplasia in 170 patients". Cancer. 56 (2): 403–12. doi:10.1002/1097-0142(19850715)56:2<403::AID-CNCR2820560233>3.0.CO;2-X. PMID 4005805.
  7. ^ a b Howard A Zacur; Robert L Giuntoli, II; Marcus Jurema. "Endometrial Hyperplasia". UpToDate Online. Retrieved 2007-05-26.
  8. ^ Doherty, Michelle T.; Sanni, Omolara B.; Coleman, Helen G.; Cardwell, Chris R.; McCluggage, W. Glenn; Quinn, Declan; Wylie, James; McMenamin, Úna C. (2020). "Concurrent and future risk of endometrial cancer in women with endometrial hyperplasia: A systematic review and meta-analysis". PLOS ONE. 15 (4): e0232231. Bibcode:2020PLoSO..1532231D. doi:10.1371/journal.pone.0232231. PMC 7188276. PMID 32343732.
  9. ^ Lacey, James V.; Sherman, Mark E.; Rush, Brenda B.; Ronnett, Brigitte M.; Ioffe, Olga B.; Duggan, Máire A.; Glass, Andrew G.; Richesson, Douglas A.; Chatterjee, Nilanjan; Langholz, Bryan (2010-02-10). "Absolute risk of endometrial carcinoma during 20-year follow-up among women with endometrial hyperplasia". Journal of Clinical Oncology. 28 (5): 788–792. doi:10.1200/JCO.2009.24.1315. ISSN 1527-7755. PMC 2834395. PMID 20065186.
  10. ^ Kurman, R. J.; Kaminski, P. F.; Norris, H. J. (1985-07-15). "The behavior of endometrial hyperplasia. A long-term study of "untreated" hyperplasia in 170 patients". Cancer. 56 (2): 403–412. doi:10.1002/1097-0142(19850715)56:2<403::aid-cncr2820560233>3.0.co;2-x. ISSN 0008-543X. PMID 4005805.
  11. ^ Suh-Burgmann, Elizabeth; Hung, Yun-Yi; Armstrong, Mary Anne (September 2009). "Complex atypical endometrial hyperplasia: the risk of unrecognized adenocarcinoma and value of preoperative dilation and curettage". Obstetrics and Gynecology. 114 (3): 523–529. doi:10.1097/AOG.0b013e3181b190d5. ISSN 0029-7844. PMID 19701030. S2CID 23542620.
  12. ^ Giede, Kurt Christopher; Yen, Tin-Wing; Chibbar, Rajni; Pierson, Roger A. (October 2008). "Significance of concurrent endometrial cancer in women with a preoperative diagnosis of atypical endometrial hyperplasia". Journal of Obstetrics and Gynaecology Canada. 30 (10): 896–901. doi:10.1016/S1701-2163(16)32969-3. ISSN 1701-2163. PMC 2891955. PMID 19038073.
[edit]