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BMC Cancer

, 19:798 | Cite as

Malignant transformation of vaginal adenosis to clear cell carcinoma without prenatal diethylstilbestrol exposure: a case report and literature review

  • Lihong Pang
  • Lei LiEmail author
  • Lan Zhu
  • Jinghe Lang
  • Yalan Bi
Open Access
Case report
Part of the following topical collections:
  1. Surgical oncology, cancer imaging, and interventional therapeutics

Abstract

Background

We report an extremely rare case of vaginal clear cell carcinoma, which originated from the malignant transformation of vaginal adenosis without prenatal diethylstilbestrol (DES) exposure.

Case presentation

In this case, the patient was a Chinese woman with a history of two decades of intermittent vaginal pain, sexual intercourse pain and vaginal contact bleeding. On September 1, 2011, when the patient was 39 years old, a vaginal biopsy revealed vaginal adenosis. After intermittent drug and laser treatment, her symptoms did not improve. Four years later, on March 4, 2015, another vaginal biopsy for abnormal vaginal cytology revealed atypical vaginal adenosis. After treatment with sirolimus, her symptoms and abnormal vaginal cytology results persisted, and she underwent laparoscopic hysterectomy with bilateral salpingo-oophorectomy and excision of the vaginal lesions. One year after the hysterectomy, on August 15, 2017, the vaginal cytology results suggested atypical glandular cells, and a biopsy revealed vaginal clear cell carcinoma originating from the atypical vaginal adenosis. A wide local resection of the vaginal lesions was performed, followed by concurrent chemoradiotherapy. Regular follow-up over 16 months showed no evidence of the recurrence of vaginal adenosis or cancer.

Conclusions

Based on the evolution of a series of pathological evidence, we report the fourth case in the world of vaginal clear cell carcinoma originating from vaginal adenosis without prenatal DES exposure. Wide local excision with radiotherapy provided at least 16 months of disease-free survival.

Keywords

Vaginal adenosis Vaginal clear cell carcinoma Pathology Cytology Radiotherapy 

Abbreviations

ASC-H

Atypical squamous cells, cannot exclude high-grade squamous intraepithelial lesions

DES

Prenatal diethylstilbestrol

HPV

Human papillomavirus

HR

Homologous recombination

HSIL

High-grade squamous intraepithelial lesion

Background

Vaginal adenosis is defined as the presence of residual Mullerian ducts, which are considered remnants of the accessory mesonephric duct from the embryonic period [1], in the vaginal wall and superficial stroma of the vagina after complete vaginal development [2]. The persistence of Mullerian cells altered at the subcellular level could form the basis for the development of carcinoma in later life with a history of maternal ingestion of estrogens [3]. In November 1971, an association of the use of diethylstilbestrol (DES) during pregnancy with the subsequent development of vaginal adenocarcinoma in exposed offspring was announced [4]. Numerous studies and databases have reported and registered cases of vaginal and cervical clear cell carcinoma originating from vaginal adenosis caused by DES. However, primary vaginal clear cell carcinoma without prenatal DES exposure is very rare. To the best of our knowledge, there have only been three cases of vaginal clear cell carcinoma due to the potential malignant transformation of vaginal adenosis or atypical vaginal adenosis without prenatal DES exposure in the English literature [5, 6, 7]. In this study, we report the fourth case and review the relevant studies in the literature.

Case presentation

The patient in this report provided consent for its publication. The Institutional Review Board of Peking Union Medical College Hospital approved this study. The patient was a 45-year-old postmenopausal Han Chinese woman, gravida 5, para 2, who presented with intermittent vaginal pain, sexual intercourse pain and contact vaginal bleeding for 20 years. Her menstruation was regular with mild dysmenorrhea and a visual analog scale score of 4 of 10. Details of the diagnosis and treatments are listed in Table 1. She had absolutely no prenatal exposure to DES or any other type of estrogen. DES was never introduced into the Chinese market, and her parents stated that they did not have access to it during the Cold War, which was an era of prevalent DES use.
Table 1

Chronicle of the diagnosis and treatment. HPV, human papillomavirus

Date

Procedures of diagnosis and treatment

Pathological findings

September 1, 2011

Vaginal biopsy

Vaginal adenosis

December 16, 2011

Vulvar biopsy

Chronic inflammation; absence of focal epithelial absence; granulation tissue formation

March 4, 2013

Cytology

A few atypical glandular cells and high-grade squamous intraepithelial lesion

March 4, 2013

High-risk HPV test

Negative

April 10, 2013

Vaginal and cervical biopsy

chronic inflammation; cervical intraepithelial neoplasia of grade I

May 10, 2013

Fractional curettage

Endometrium of late proliferative phase

March 4, 2015

Cytology

Atypical squamous cells: cannot exclude high-grade squamous intraepithelial lesion

March 4, 2015

Vaginal biopsy

Vaginal adenosis; moderate atypical hyperplasia of focal squamous epithelium

December 24, 2015

Cytology

A few atypical gland cells

December 24, 2015

High-risk HPV test

Negative

March 18, 2016

Cytology

Suspicious adenocarcinoma of cervix; atypical squamous epithelial cells of vagina

March 3, 2016

Fractional curettage

A little cervical canal tissue and endometrium of secretory phase

April 15, 2016

Vaginal biopsy

The serous papillary glands with active growth; chronic inflammation

May 4, 2016

Hysterectomy with bilateral salpingoophorectomy, and excision of vaginal lesions

Normal findings except atypical vaginal adenosis in the vaginal wall

May 15, 2017

Cytology

A few atypical gland cells

May 15, 2017

Biopsy of vaginal stump

Serous papillary glands with active growth, which suggested atypical adenosis

August 15, 2017

Excision of vaginal lesions

The mass of mid-anterior vaginal wall was confirmed to be clear cell carcinoma

September 15, 2017

Wide local resection of vaginal lesions

Atypical vaginal adenosis with negative incision margin

July 18, 2018

Biopsy of vulvar ulcer

Chronic inflammation of fibrous tissue and squamous epithelium

Discovery and treatment of vaginal adenosis (September 2011 to December 2015)

On September 1, 2011, at age 39, the patient underwent a vaginal biopsy due to a vaginal ulcer found through physical examination. The pathological findings revealed vaginal adenosis. After 3 months of treatment with tacrolimus, the ulcerative lesion persisted. A biopsy of a 2-cm hypopigmented area of the medial right minor labia was performed, and the pathological findings revealed chronic inflammation with granulation formation. Later, two laser treatments were performed for the vaginal adenosis and vulvar lesions, and remission was achieved after the treatment. On March 4, 2013, the patient went to the outpatient clinic due to aggravated vaginal pain. On physical examination, her bilateral minor labia were slightly edematous with thinned mucosa, but the vagina appeared normal. A cervical cytology test revealed a high-grade squamous intraepithelial lesion (HSIL), and her high-risk human papillomavirus (HPV) test result was negative. Subsequently, a cervical biopsy and fractional curettage revealed grade I cervical intraepithelial neoplasia and normal endometrium of the late proliferative phase. No further surgical interventions were performed, such as loop electrosurgical excision or conization. She underwent 2 months of treatment with sirolimus (rapamycin). On March 4, 2015, she came to the hospital due to vaginal pain and an inability to have sexual intercourse. A physical examination revealed that the lower third of the vaginal mucosa was swollen with an erosive lesion 0.5 cm in diameter. Her cervical cytology results showed ASC-H (atypical squamous cells, cannot exclude HSILs). A biopsy revealed vaginal adenosis with moderate atypical hyperplasia of the focal squamous epithelium (Fig. 1). She was treated with sirolimus for another two months. The symptoms did not improve; she stopped taking the medicine and was transferred to the unit of the authors.
Fig. 1

Vaginal biopsy on March 4, 2015 revealed vaginal adenosis (hematoxylin and eosin staining, × 10)

Discovery and treatment of atypical vaginal adenosis (December 2015 to August 2017)

On December 24, 2015, the vaginal cytology results showed suspicious adenocarcinoma and atypical squamous epithelial cells. Another biopsy of the visible vaginal lesion suggested serous papillary glands with active growth. She underwent laparoscopic hysterectomy, bilateral salpingo-oophorectomy, and excision of the vaginal lesions on May 4, 2016. The postoperative pathology revealed atypical vaginal adenosis (Fig. 2). Twelve months after the hysterectomy, on May 15, 2017, her physical examination revealed polypoid tissue on the anterior vaginal wall, and vaginal biopsy revealed vaginal atypical adenosis (Fig. 3).
Fig. 2

Excision of vaginal lesions on May 4, 2016 revealed atypical vaginal adenosis (hematoxylin and eosin staining, a, × 10; b, × 50)

Fig. 3

Biopsy of vaginal stump on April 15, 2017 revealed atypical vaginal adenosis (hematoxylin and eosin staining, × 10)

Discovery and treatment of vaginal clear cell carcinoma (August 2017 to December 2017)

On August 15, 2017, excision of the visible vaginal lesions revealed clear cell carcinoma of the vagina (Fig. 4a, b) and coexisting lesions of atypical adenomyosis (Fig. 4c). On September 15, 2017, she underwent wide local resection of the vagina, and the postoperative pathology results showed atypical vaginal adenosis with a negative margin and without residual carcinoma. Stage I vaginal clear cell carcinoma was confirmed. She underwent brachytherapy (30 Gy, five times) and concurrent cisplatin chemotherapy from October to December 2017. Since the patient refused external radiotherapy, concurrent cisplatin chemotherapy was applied only once (60 mg, intravenous). In October 2017, she provided samples for germline and somatic sequencing using a multi-gene panel of 57 gene mutations, including most genes involved in homologous recombination (HR) and non-HR pathways, such as BRCA 1/2, RAD51C, PTEN, TP53, VHL, BAP1, SETD2, PBRM1, and MTOR. No deleterious variants or variants of unknown significance were discovered.
Fig. 4

Excision of visible lesions in the mid-anterior vaginal wall on August 15, 2017 revealed clear cell carcinoma (hematoxylin and eosin staining, a, × 10; b, × 20) and coexisting atypical vaginal adenosis (hematoxylin and eosin staining, c, × 4)

Follow-up (December 2017 to the present)

The patient participated in regular follow-up examinations. On July 18, 2018, she underwent a vulvar biopsy because of a vulvar ulcer. The pathological findings revealed inflammation, which improved after treatment with topical hormones. Her symptoms have since been relieved. Her progression-free survival of vaginal cancer reached 20 months in January 2019.

Discussion

Primary vaginal malignancies are very rare, accounting for approximately 2% of all female genital malignancies [8]. More than 80% of vaginal cancers are squamous cell carcinomas [9]. Vaginal clear cell carcinoma is a rare type of vaginal cancer that usually occurs in women whose mothers used DES during pregnancy [10]. However, there have only been three known cases of vaginal clear cell carcinoma without prenatal DES exposure, most likely due to the malignant transformation of vaginal adenosis or atypical vaginal adenosis (Table 2) [5, 6, 7]. In the report by Uehara et al. [5], a 54-year-old woman complained of a 3-month history of genital bleeding, and the examination revealed clear cell adenocarcinoma at the anterior vagina, congenital anomalies of the bicornuate uterus and vaginal septum, and left ureteral agenesis. The patient was well without recurrence at 43 months after anterior pelvic exenteration. In the report by Satou et al. [6], another patient died of disease 16 months after radical hysterectomy and chemotherapy. In the report by Prasad et al. [7], the tumor, whose features were found to be similar to those of small cell carcinomas arising elsewhere in the female genital tract, was studied by light and electron microscopy and immunohistochemistry; intracytoplasmic electron-dense neurosecretory-type granules were observed, and immunohistochemistry revealed chromogranin A. The current report describes the fourth case, in which a definite evolution from vaginal adenosis to atypical vaginal adenosis and ultimately to clear cell carcinoma was observed.
Table 2

Cases of vaginal clear cell carcinoma due to the potential malignant transformation of vaginal adenosis or atypical vaginal adenosis without prenatal DES exposure in the English literature

Reference

Age at diagnosis of carcinoma

Atypical adenosis

Congenital anomalies

Courses from adenosis to carcinoma

Treatment

Disease-free survival

Overall survival

Recurrence

Mortality

Uehara T et al. [5]

54 years

None

Bicornuate uterus and vaginal septum and left ureteral agenesis

3 months

Anterior pelvic exenteration

43 months

43 months

No

No

Satou Y et al. [6]

38 years

None

Didelphys uterus, duplicated and imperforated vagina

Not available

Radical hysterectomy and chemotherapy

Not available

16 months

Not available

Yes

Prasad CJ [7]

34 years

Yes

None

Not available

Vaginectomy with bilateral inguinal lymph node dissection, chemotherapy of cisplatin and etoposide, teletherapy, brachytherapy

Not available

6 months

With tumor noted at deep margins of the vagina

Yes

Case in the report

45 years

Yes

None

6 years

Hysterectomy, wide local resection of vaginal lesion, and brachytherapy

16 months

16 months

No

No

The exact pathogenesis of the malignant transformation of vaginal adenosis without prenatal DES exposure is unknown. A study of clear cell carcinoma in women exposed prenatally to DES revealed the presence of both cervical ectropion and vaginal adenosis in all 20 specimens, and tubo-endometrial glands were intimately related to the carcinoma in 18 of the 20 cases, suggesting that the tubo-endometrial epithelium, whether in the ectocervix or vagina, serves as a source for the development of clear cell adenocarcinoma [11]. The frequency with which atypical tubo-endometrial glands in the vagina and cervix are associated with these carcinomas and the proximity of the former to the latter provide strong evidence that atypical vaginal adenosis and atypical cervical ectropion of the tubo-endometrial type are precursors of clear cell adenocarcinoma [12]. Lewis et al. [13] consistently found aneuploidy in 3 cases of invasive clear cell carcinoma of the vagina, suggesting that the immediate precursor state should also be in the aneuploid range. The 3 adenosis specimens, however, were in the normal diploid to tetraploid range. Aside from the toxicity of DES exposure, chemotherapeutic drugs may play a role in promoting the occurrence of vaginal adenosis and carcinoma. Cases of vaginal adenosis after topical 5-fluorouracil therapy for vaginal HPV-associated lesions [14] and vaginal adenosis together with clear cell carcinoma after 5-fluorouracil treatment for condylomas [15] have been reported. Congenital anomalies of the genitourinary tract have been suspected as the cause of clear cell carcinoma without DES exposure [5], which has been disputed [16]. Although there is a case report of adenocarcinoma originating from metanephric remnants [17], it is unlikely that it originated from clear cell carcinoma because of the topographical dissimilarity [18]. Currently, objective findings suggest that human prenatal epithelialization of the cervix and vagina results in 3 morphogenetically determined units [19], which may provide new insight into the histogenesis and transformation of vaginal adenosis.

In our report, before the discovery of adenosis, the patient had undergone multiple medical and invasive treatments, including treatment with tacrolimus and sirolimus, laser treatment and repeated biopsies. Whether these medical regimens and procedures would prompt the production of atypical adenosis or a transformation to vaginal cancer requires further exploration. Although there have been no reports on the relationship between trauma or medical treatments, except for diethylstilbestrol, and the transformation of adenosis, an off-label and unreasonable application of medicine should be avoided.

The natural history from vaginal adenosis to cancer varies greatly. Most patients with vaginal adenosis have no obvious symptoms. The lesions range widely, and symptoms can manifest as postcoital hemorrhage, sexual pain and a vaginal burning sensation [20]. In some cases, vaginal palpation reveals submucous nodular or sandy lesions 0.5–5 cm in diameter [20]. However, the main clinical manifestations of vaginal cancer include irregular vaginal bleeding, postpartum hemorrhage, postmenopausal hemorrhage and increased leucorrhea. The most common type of local vaginal lesions is the papillary or cauliflower type, followed by the ulcerative or infiltrative type. Difficulty in sexual intercourse is a typical symptom of advanced vaginal tumors.

Vaginal adenosis and clear cell carcinoma often occur several years after exposure to DES in the uterine cavity. Non-DES-induced vaginal adenosis has a reported incidence of approximately 10% in adult women. In the present case, the patient’s mother did not use DES during pregnancy since DES was never introduced into the Chinese market. Vaginal clear cell carcinoma was identified 6 years after the discovery of vaginal adenosis. A consensus regarding the detection and diagnosis of atypical vaginal adenosis and/or vaginal clear cell carcinoma is lacking. Cytology has been clinically valuable in proving cases of vaginal adenosis and adenocarcinoma [21]. Colposcopy with biopsy for abnormal vaginal and/or cervical cytology results could reveal possible lesions, as described in our report.

Laser therapy, cryotherapy and cautery can be used to treat superficial and small lesions of vaginal adenosis [22]. The lesions can also be coated topically with 10–20% silver nitrate or potassium dichromate solution for lesion necrosis and exfoliation. For a single localized submucosal lesion, complete resection of the lesion can be performed. For those with severe atypical hyperplasia or malignant transformation, the principle of treatment is the same as for those with vaginal cancer, despite a lack of sufficient evidence [23]. On the other hand, radiotherapy is the first choice for some patients with early or advanced vaginal cancer [24]. Radiotherapy includes brachytherapy and external beam. The use of brachytherapy in vaginal cancer imparts a benefit in terms of disease-specific and overall survival [25, 26]. The treatment of vaginal cancer with a multichannel cylinder produces high local control [27]. Surgery is also an option for patients with early-stage primary vaginal cancer [28]. Patients with early-stage vaginal tumors without deep infiltration may undergo radical hysterectomy, partial vaginal resection and pelvic lymphadenectomy. The margin of vaginal resection should be 2–3 cm beyond the tumor. For vaginal midsegment tumors, in addition to total vaginal hysterectomy, inguinal lymph node or pelvic lymph node resection should be performed according to the size of the lesion and the location of lymph node metastasis [29]. Total vaginal resection, including rectal resection or cystectomy (pelvic exenteration), is necessary for treatment, but the operation is extremely complicated [30, 31]. The effect of chemotherapy has been shown to be minimal. In the case reported by Satou et al. [6], the patient survived only 16 months after radical hysterectomy and chemotherapy. However, in the current case, several inappropriate therapy protocols were applied. Before being transferred to our unit, the patient was treated with tacrolimus and sirolimus, neither of which had definite indications or resulted in symptomatic relief. Although there have been several reports on the application of tacrolimus for the treatment of erosive lichen planus [32, 33, 34], these experiences are not applicable to the treatment of adenosis.

In conclusion, we report the fourth case in the world of vaginal clear cell carcinoma stemming from the malignant transformation of vaginal adenosis without prenatal DES exposure, with serial evidence of oncological evolution. Wide local excision with radiotherapy provided at least 16 months of disease-free survival. Serial follow-up examinations with vaginal cytology is essential for patients with vaginal adenosis for the diagnosis of atypical lesions and even cancer.

Notes

Acknowledgements

Not applicable.

Authors’ contributions

LL and LP planned and designed the analysis and contributed to the acquisition of data. LZ and JL contributed to the acquisition of data, interpretation of the analysis results and critical revision of the manuscript for important intellectual content. YB reviewed and provided the pathological outcomes. All authors have read and approved the final manuscript.

Funding

This study was supported by the Chinese Academy of Medical Sciences Initiative for Innovative Medicine (CAMS-2017-I2M-1-002) and by the National Science-technology Support Plan Projects (2015BAI13B04). The funders played no role in the study design, data collection or analysis, decision to publish, or manuscript preparation.

Ethics approval and consent to participate

The patient in this report provided consent for participation in the study. The Institutional Review Board of Peking Union Medical College Hospital approved this study.

Consent for publication

The patient in this report provided consent for the publication of her experiences in an anonymous style. A copy of the patient’s consent to publication form is available to the Editor of the journal. All authors of this report agree with and are greatly obliged to the Editorial Board of BMC Cancer for the publication of this report.

Competing interests

The authors declare that they have no competing interests.

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Copyright information

© The Author(s). 2019

Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.

Authors and Affiliations

  1. 1.Department of Obstetrics and Gynecology, Peking Union Medical College HospitalPeking Union Medical College & Chinese Academy of Medical ScienceBeijingChina
  2. 2.Department of Pathology, Peking Union Medical College HospitalPeking Union Medical College & Chinese Academy of Medical ScienceBeijingChina

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