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Route-specific association of progestin therapy and concurrent metformin use in obese women with complex atypical hyperplasia
  1. Koji Matsuo1,2,
  2. Rachel S Mandelbaum1,
  3. Marcia Ciccone1,2,
  4. Mahdi Khoshchehreh1,
  5. Heena Purswani1,
  6. Elise B Morocco1,
  7. Shinya Matsuzaki1,
  8. Christina E Dancz1,
  9. Begum Ozel1,
  10. Richard J Paulson1 and
  11. Lynda Roman1,2
  1. 1Obstetrics and Gynecology, University of Southern California, Los Angeles, California, USA
  2. 2Division of Gynecologic Oncology, Department of Obstetrics and Gynecology, University of Southern California, Los Angeles, California, USA
  1. Correspondence to Dr Koji Matsuo, Division of Gynecologic Oncology, Department of Obstetrics and Gynecology, University of Southern California, Los Angeles, CA 90033, USA; koji.matsuo{at}gmail.com

Abstract

Introduction Previous studies have suggested that metformin use may enhance the therapeutic effect of progestin therapy for endometrial hyperplasia or malignancy. However, it is not known how the impact of concurrent metformin may be altered by route of progestin therapy, either locally via an intrauterine device or systemically. This study examined the effectiveness of concurrent metformin use and progestin therapy for women with complex atypical hyperplasia stratified by progestin route (systemic vs local).

Methods This single-institution retrospective study examined consecutive women with complex atypical hyperplasia who received progestin therapy from 2003 to 2018. Time-dependent analyses for complete response rate were performed comparing concurrent metformin users versus non-users in the oral progestin group and in the levonorgestrel-releasing intrauterine device group.

Results Across the study cohort (n=245), there were 137 (55.9%) women who responded to progestin therapy. In the oral progestin group (n=176), the median age and body mass index were 36 years and 37.7 kg/m2, respectively. 36 (20.5%) of women on oral progestins also took metformin. After controlling for diabetes status, women taking both oral progestins and metformin had a complete response rate similar to those not taking metformin (6 month cumulative rates, 23.1% vs 27.8%, adjusted hazard ratio (aHR) 0.71, 95% confidence interval (95% CI) 0.36 to 1.41). In the levonorgestrel-releasing intrauterine device group (n=69), the median age and body mass index were 35 years and 39.9 kg/m2, respectively. There were 15 (21.7%) women who took metformin in addition to the levonorgestrel-releasing intrauterine device. After controlling for diabetes status, women who had the levonorgestrel-releasing intrauterine device and took metformin had a significantly higher complete response rate compared with those not taking metformin (6 month cumulative rates, 86.7% vs 58.9%, aHR 2.31, 95% CI 1.09 to 4.89).

Conclusion In a predominantly obese population, concurrent metformin may possibly offer treatment benefit when used with the levonorgestrel-releasing intrauterine device.

  • endometrial hyperplasia

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HIGHLIGHTS

  • In women taking oral progestins, concurrent metformin does not impact treatment response.

  • Concurrent metformin was associated with improved response in women using the levonorgestrel-releasing intrauterine device.

  • Effectiveness of concurrent metformin for complex atypical hyperplasia may depend on the progestin route.

Introduction

Complex atypical hyperplasia is a pathological pre-malignant lesion in the endometrium and is a precursor of endometrial cancer.1 2 Nearly 30% of women with complex atypical hyperplasia have progression to endometrial cancer, and up to 40% of women diagnosed with complex atypical hyperplasia are found to have an occult endometrial cancer at the time of hysterectomy.1–3 Total hysterectomy is the standard definitive treatment for complex atypical hyperplasia1; however, reproductive-aged women who desire future fertility or those who are poor surgical candidates may undergo medical treatment with progestin therapy.1 Progestin therapy for complex atypical hyperplasia can be highly effective; nearly two thirds of women show complete regression.4 5 The remaining one third who have treatment failure with progestin therapy require additional or alternative treatment, even hysterectomy. One such strategy to overcome progestin-resistant complex atypical hyperplasia may be the adjunctive use of metformin concurrently with progestin therapy.

Metformin is an insulin-sensitizing biguanide commonly used in the treatment of type 2 diabetes mellitus.6 Pre-clinical studies have shown anti-tumor activity via the mammalian target of rapamycin pathway in endometrial cancer.7 8 A prior clinical study also suggested that metformin may enhance the therapeutic effect of oral progestin therapy for women with atypical endometrial hyperplasia or malignancy (>80% complete regression rate).9 However, this trial lacked an active comparator, making their results difficult to interpret. Another trial with similar results had a control group but was fairly limited due to sample size (n=16).10 Moreover, a 2017 systematic review remarked that there remains an insufficient body of evidence to support the pharmaco-adjunctive use of metformin with oral progestin in endometrial hyperplasia.11

Recently, several studies have suggested that the effectiveness of progestin therapy for complex atypical hyperplasia may differ by treatment route, and local progestin therapy may be more effective than systemic therapy, particularly in obese individuals.12 13 Based on available data, we hypothesized that the effectiveness of concurrent metformin may differ depending on route of progestin therapy (systemic vs local). The objective of the current study was to examine the effectiveness of concurrent metformin use and progestin therapy for complex atypical hyperplasia in a predominantly obese population, stratified by progestin route (systemic vs local).

Methods

Data Source and Eligibility

This is a secondary exploratory analysis of a previously conducted retrospective study examining consecutive women with complex atypical hyperplasia who received treatment at the Los Angeles County Medical Center from 2003 to 2018.13 14 Institutional Review Board approval at the University of Southern California was properly obtained (HS-11–00131). The study population comprised 245 women who were diagnosed with complex atypical hyperplasia and who received medical treatment with progestins . These women had received at least 1 month of progestin therapy (either oral or local) following the complex atypical hyperplasia diagnosis. Women with non-atypical or simple hyperplasia or endometrial cancer were excluded. Additionally, those who received multiple progestins or progestin therapy before the complex atypical hyperplasia diagnosis were excluded. Finally, women who did not have a follow-up biopsy performed at least 1 month following treatment initiation were excluded from the study.

Clinical Information

Variables recorded in the database included patient demographics, medical comorbidities, medication types, treatment response, and follow-up. Patient demographics at the initial complex atypical hyperplasia diagnosis included age, year, race/ethnicity, gravidity, parity, and body mass index. Endometrial thickness on ultrasonographic imaging at the time of complex atypical hyperplasia diagnosis was also abstracted. Medical comorbidities included diabetes mellitus, hypertension, hyperlipidemia, polycystic ovary syndrome, and reported infertility. Medication types included metformin, aspirin, statins, and β-blockers at the time of complex atypical hyperplasia diagnosis.

Progestin route of administration was grouped as systemic versus local based on the first-line agent used after the initial diagnosis of complex atypical hyperplasia. Systemic progestins included oral medroxyprogesterone acetate, megestrol acetate, norethindrone, or intramuscular depo-medroxyprogesterone acetate (termed oral progestin group). Local therapy was defined as treatment with the levonorgestrel-releasing intrauterine device.

Treatment Follow-Up

In our practice, re-sampling of the endometrium is usually performed every 3 to 6 months in those who elect for medical management to assess treatment response. In those who achieve complete response, follow-up is generally continued in the same fashion but can be personalized, depending on specific patient risk factors or clinical considerations. Date of treatment initiation and last follow-up date were recorded. The chronologic sequence of complex atypical hyperplasia diagnosis, progestin therapy initiation, and treatment outcomes on follow-up endometrial biopsies were then ascertained from this information.

Study Definition

Body mass index was classified as: overweight (25–29.9 kg/m2), class I obesity (30–34.9 kg/m2), class II obesity (35–39.9 kg/m2), and class III obesity (≥40 kg/m2).15 Histopathology diagnoses of endometrial hyperplasia were based on the 1994 World Health Organization criteria as: simple hyperplasia without atypia, simple hyperplasia with atypia, complex hyperplasia without atypia, and complex hyperplasia with atypia.2

Response for progestin therapy was categorized as: complete response, defined as no residual hyperplasia identified on subsequent biopsies; partial response, defined as regression of complex atypical hyperplasia to simple or non-atypical hyperplasia; persistent disease; and progression to cancer. Overall response refers to complete response and partial response. Time to treatment response was defined as the time interval between initiation of progestin therapy and the first follow-up biopsy demonstrating treatment response. The last follow-up was defined as the time interval between progestin therapy initiation and the last endometrial biopsy. Cases were censored at the last follow-up if an outcome event was absent. Women who changed progestin therapy route, changed to a different progestin agent, initiated combination progestin therapy, or underwent hysterectomy were censored at those time points.

Statistical Consideration

The primary objective of the analysis was to examine the effectiveness of concurrent metformin use during progestin therapy stratified by route of progestin administration (systemic vs local). The study cohort was grouped as oral progestin versus levonorgestrel-releasing intrauterine device. In each cohort, women were divided based on metformin use (users vs non-users), and treatment response was assessed. The secondary aim was to identify the characteristics associated with metformin use.

Differences in baseline demographics between the two groups were assessed with the Mann-Whitney U test, Fisher exact test, or χ2 test as appropriate. A binary logistic regression model was fitted to identify the independent characteristics associated with metformin use. The conditional backward method was used to retain only covariates with a p<0.05 level in the final model due to limited sample size. The effect size of statistical significance was expressed with odds ratio and 95% confidence interval (OR, 95% CI).

As treatment response to progestin therapy depends on follow-up duration, a time-dependent analysis was performed to assess progestin treatment response. Cumulative response curves were plotted with the Kaplan-Meier method, and differences in curves were assessed with the log-rank test. A Cox proportional hazard regression model was then used to estimate the effect size of metformin use on progestin therapy route and treatment response (complete response and overall response). A parsimonious adjustment model was fitted for this multivariable analysis, and the association between metformin use and treatment response was adjusted for independent factors associated with metformin use in each cohort. In an additional adjustment, the association was controlled for body mass index. This was based on the post-hoc assessment of the study population that showed different body habitus per treatment allocations. The effect size of statistical significance was expressed with adjusted hazard ratio (aHR) and 95% CI.

All statistical analyses were based on two-sided hypotheses, and p<0.05 was considered statistically significant. Statistical Package for Social Sciences (SPSS, version 25.0, Armonk, NY, USA) was used for all analyses. The STROBE (STrengthening the Reporting of OBservational studies in Epidemiology) guidelines were utilized to outline this observational cohort study.16

Results

Systemic Progestin Cohort

Across the study cohort (n=245), there were 137 (55.9%) women who responded to progestin therapy. There were 176 women who received systemic progestin treatment for complex atypical hyperplasia. Patient demographic characteristics are shown in Table 1. The median age and body mass index were 36 years and 37.7 kg/m2, respectively. The majority of women were obese (n=147, 83.5%), and nearly half were nulligravid (n=90, 51.1%). Diabetic women represented nearly one third of this group (n=56, 31.8%).

Table 1

Patient demographics (systemic progestin group)

In the systemic progestin cohort, 36 (20.5%) women used concurrent metformin and the remaining 140 (79.5%) women received progestin therapy alone. In univariable analysis (Table 1), women who received metformin were more likely to have diagnoses of diabetes (77.8% vs 20.0%), dyslipidemia (61.1% vs 11.4%), and/or polycystic ovary syndrome (33.3% vs 14.3%), and were more likely to also use a statin (22.2% vs 4.3%), compared with those who did not use metformin (all, p<0.05). On multivariable analysis (Table 1), diabetes mellitus (adjusted OR (aOR) 12.5, 95% CI 4.21 to 37.4), hyperlipidemia (aOR 6.29, 95% CI 2.33 to 16.9), and polycystic ovary syndrome (aOR 6.20, 95% CI 1.83 to 21.1) remained independent factors associated with metformin use (all, p<0.05).

The median follow-up time was 9.0 months (IQR 3.5–31.1), and there were 60 (34.1%) women who had a complete response and 18 (10.2%) women who had a partial response (overall response, n=78, 44.3%). On univariable analysis (Figure 1A), metformin users had a cumulative complete response rate similar to those of non-users (6 month cumulative rates, 23.1% vs 27.8%, and 1 year cumulative rates, 40.8% vs 45.8%, p=0.384). After controlling for diabetes status (Figure 2), metformin use was not associated with complete response (aHR 0.71, 95% CI 0.36 to 1.41; p=0.326). When controlling for body mass index, concurrent metformin was not associated with complete response (aHR 0.74, 95% CI 0.38 to 1.46; p=0.390). Similarly, metformin use was not associated with overall response (online supplementary figure S1A and S2).

Supplemental material

Figure 1

Cumulative complete response (CR) rate per metformin use. Log-rank test for p values. Cumulative rate of CR is compared with metformin users and non-users in (A) oral progestin therapy and (B) levonorgestrel-releasing intrauterine device (LNG-IUD) therapy.

Figure 2

Adjustment models for association between metformin use and complete response (CR) (systemic progestin and levonorgestrel-releasing intrauterine device (LNG-IUD) cohorts). Cox proportional hazard regression test for adjustment models. Circles represent hazard ratio for the likelihood of CR or partial response (PR) with metformin compared with non-metformin. Bars represent 95% confidence interval. *P<0.05. BMI, body mass index; DM, diabetes mellitus; HLD, hyperlipidemia, PCOS, polycystic ovarian syndrome.

Local Progestin Cohort

There were 69 women who received the levonorgestrel-releasing intrauterine device for the treatment of complex atypical hyperplasia. Patient demographic characteristics are shown in Table 2. The median age and body mass index were 35 years and 39.9 kg/m2, respectively. Nearly half of women in this group were morbidly obese (class III obesity, n=34, 49.3%) and nearly half were nulligravid (n=37, 53.6%). Nearly one quarter of the group was diabetic (n=18, 26.1%).

Table 2

Patient demographics (levonorgestrel-releasing intrauterine device group)

In the levonorgestrel-releasing intrauterine device group (n=69), there were 15 (21.7%) women who took metformin in addition to the levonorgestrel-releasing intrauterine device, and the remaining 54 (78.3%) women did not. On univariable analysis (Table 2), metformin users were more likely to have diabetes (73.3% vs 13.0%), dyslipidemia (53.3% vs 20.4%), and/or infertility (60.0% vs 27.8%) compared with non-users (all, p<0.05). On multivariable analysis (Table 2), diabetes mellitus (aOR 20.5, 95% CI 4.52 to 93.2) and infertility (aOR 4.68, 95% CI 1.03 to 21.3) remained independent factors associated with metformin use (both, p<0.05).

The median follow-up time in the levonorgestrel-releasing intrauterine device group was 9.8 months (IQR 4.1–23.3); there were 58 (84.1%) women who had a complete response and one (1.4%) woman who had a partial response (overall response, n=59, 85.5%). On univariable analysis (Figure 1B), metformin users had a significantly higher cumulative complete response rate compared with non-users (6 month cumulative rates, 86.7% vs 58.9%, and 1 year cumulative rates, 100% vs 80.7%, p=0.007). After controlling for diabetes status (Figure 2), metformin users had a twofold increased likelihood of achieving complete response (aHR 2.31, 95% CI 1.09 to 4.89; p=0.030). After controlling for body mass index, metformin use was significantly associated with increased likelihood of achieving complete response (aHR 2.35, 95% CI 1.24 to 4.43; p=0.008). Similar results were observed for overall response (online supplementary figure S1B and S2).

Discussion

A key finding of the current study is that the benefit of concurrent metformin may differ depending on the route of progestin therapy for complex atypical hyperplasia, particularly in obese women. Among women who received systemic progestin treatment, concurrent metformin was not associated with improved treatment response, whereas in women using local progestin therapy, treatment response was improved with the addition of metformin. Possible direct and indirect associations between progestin and metformin merit further discussion.

These findings suggest that systemic progestins may possibly limit any added benefit of concurrent metformin therapy. Metformin is typically given orally; thus, there is a possibility of a direct drug–drug interaction with oral progestins in the systemic circulation. In general, metformin-related drug–drug interaction involves transporters in enterocytes, hepatocytes, and tubular cells via multidrug and toxin extrusion transporter, organic cation transporter, and plasma membrane monoamine transporter.17 Thus, if progestin interacts with these transporters, it is possible that the metabolism of metformin could potentially be altered. A prior in vitro study showed that organic cation transporter activity may increase with progestin exposure in endometrial cancer cell lines,18 suggesting that a drug–drug interaction between metformin and oral progestin may be present via the organic cation transporter pathway. To date, in a contemporary view of literature, direct drug–drug interaction between metformin and oral progestin has not been examined but should be further investigated.17

Decreased efficacy of metformin in the systemic progestin group may also be due to indirect interactions between metformin and oral progestins. One possibility for an indirect effect is the impact of oral progestins on patients’ weight (Figure 3). A recent study showed that oral progestin use is associated with significant weight gain compared with local progestin therapy among women with complex atypical hyperplasia and endometrial cancer (2.95 kg vs 0.05 kg weight gain in 1 year).19 Therefore, increased adiposity due to weight gain from oral progestin therapy may result in an increase in inflammatory cytokines from excess adipocytes that can stimulate oncogenesis in the endometrium.20 Given the fact that metformin’s anti-tumor activity seems to be via the inhibition of circulating pro-inflammatory mediators rather than a direct anti-tumor effect, as demonstrated in a recent prospective study,21 weight gain may counteract the anti-inflammatory mechanism by which metformin exerts benefit in the setting of complex atypical hyperplasia.22

Figure 3

Hypothesis-generating schema for the interaction between metformin and systemic progestin. Possible pathways for the interaction of progestin and metformin in obesity are shown. Inflammatory cytokines from excess adiposity stimulate endometrial cells for oncogenesis. Metformin inhibits inflammatory cytokines from the adipocytes. Systemic progestin may cause weight gain, resulting in increases in inflammatory cytokines and decreases in the relative effectiveness of metformin. LNG-IUD, levonorgestrel-releasing intrauterine device.

Therefore, local progestin therapy with the levonorgestrel-releasing intrauterine device may be an attractive approach to deliver progestin while maintaining the anti-inflammatory benefits of metformin in the treatment of women with complex atypical hyperplasia. The rationale for this hypothesis is based on the following: (1) our observation demonstrating higher treatment response with metformin in the levonorgestrel-releasing intrauterine device group but not in the systemic progestin group; (2) local therapy with levonorgestrel-releasing intrauterine device does not lead to weight gain19; (3) concurrent use of metformin during progestin therapy may be more effective in women with large body habitus23; and (4) large body habitus is associated with increased recurrence risk with progestin therapy.24 The latter two rationales suggest that the anti-inflammatory effects of metformin are responsible for its anti-tumor activity, particularly in obese women who have increased inflammation from adipose tissue. This effect may be evident with the levonorgestrel-releasing intrauterine device given the absence of weight gain, while weight gain from oral progestins may mask any positive effects of metformin. Further study is definitely warranted to support this hypothesis.

There are several limitations in this study. First, there is unmeasured bias in all retrospective observational studies. For example, we are unable to know details that contributed to the decision process for route of progestin therapy. The exact indication for, timing of, and compliance with metformin therapy were also not assessable. Similarly, patient compliance, adverse effects, and weight changes related to progestin treatment were not available but likely impacted the results. Second, information regarding glycemic control in diabetic or pre-diabetic patients was not included. Also, metformin dose, frequency, and duration of treatment were not assessed but may possibly interact with the analysis. Third, the majority of this patient population was Hispanic and obese, and generalizability to patients of different race/ethnicity or body habitus is unknown. The relatively lower response rate in this study compared with other studies may be secondary to the unique characteristics of our population with a high rate of morbid obesity, historically low rates of treatment compliance, and short follow-up intervals as described previously.13 14 Fourth, while we speculated based on prior evidence that the mechanism of metformin’s anti-tumor effect is secondary to anti-inflammatory pathways in excess adipocytes, this study does not provide actual data to support this theory. Lastly, a central pathology review was not performed for the diagnostic confirmation of complex atypical hyperplasia in the study. It is possible that the relatively low response rate to progestin therapy in our study may be due to misclassification of complex atypical hyperplasia and low-grade endometrioid endometrial cancer, as distinguishing the two diagnoses can often be challenging.25 26

In summary, our study suggests that concurrent use of metformin during progestin therapy may be more effective when the progestin is given with the levonorgestrel-releasing intrauterine device. As this recommendation is based on a single study of retrospective observation, prospective studies are surely necessary to confirm this finding. There is an ongoing randomized controlled trial comparing the complete response rates of the levonorgestrel-releasing intrauterine device with and without metformin for obese women with complex atypical hyperplasia or grade 1 endometrioid adenocarcinoma of the endometrium (NCT01686126).27 The study team used an estimated complete response rate of 68% (95% CI 45% to 86%) with levonorgestrel-releasing intrauterine device treatment and assumed a 60% increase in the estimated likelihood of complete response with metformin.28 Based on their sample size estimation, 45 patients will be examined for each group. This trial will ultimately help answer questions regarding the effectiveness of metformin as an adjunct to progestin therapy in complex atypical hyperplasia.

References

Footnotes

  • KM and RSM contributed equally.

  • Correction notice Since the publication of this article, the authors have noticed that the author name ‘Heena Pursuwani’ is incorrect. The correct author name is ‘Heena Purswani’.

  • Contributors Conceptualization: KM; Data curation: RSM, MAC, MK, HP, EBM; Formal analysis: KM; Funding acquisition: KM, LDR; Investigation: all authors; Methodology: KM; Project administration: MAC, CED; Resources: all; Software: KM; Supervision: KM; Validation: KM; Visualization: KM, SM; Writing - original draft: KM; Writing - review & editing: all authors.

  • Funding This study was funded by Ensign Endowment for Gynecologic Cancer Research (KM).

  • Competing interests Consultant, Quantgene (LDR); honorarium, Chugai, textbook editorial expense, Springer, and investigator meeting attendance expense, VBL therapeutics (KM); Research funding, MSD (SM).

  • Patient consent for publication Not required.

  • Provenance and peer review Not commissioned; externally peer reviewed.

  • Data availability statement No data are available.