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. 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. 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. • 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. • 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. ==Diagnosis==