Malignant Transformation Associated with Endometrioid Adenocarcinoma of Abdominal Wall Endometriosis: A Case Report and Literature Review

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This paper describes a 39-year-old woman with a long-enlarging abdominal wall mass arising after cesarean section, evaluated with ultrasound and contrast-enhanced CT that suggested a mesenchymal-origin lesion and could not rule out degenerative leiomyoma or sarcoma. The authors performed laparoscopic exploration, resection of the abdominal wall mass with excision of invaded posterior sheath/peritoneum, and abdominal wall reconstruction, with pathology revealing highly differentiated endometrioid adenocarcinoma with squamous features and supportive immunohistochemistry; diagnostic curettage later showed atypical endometrial hyperplasia, and she received adjuvant chemotherapy. A key limitation is that preoperative diagnosis was challenging and the paper relies on postoperative histology and literature aggregation, reporting only a small number of reported endometrioid AWE cases found via a PubMed search from 1980 to April 2024. This paper is centrally about endometriosis—specifically malignant transformation of abdominal wall endometriosis into endometrioid adenocarcinoma.

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Abstract

INTRODUCTION: Endometriosis is a prevalent chronic gynecological disease, characterized by the growth of endometrial glands and stroma outside the uterus and by the presence of chronic inflammatory lesions. This condition is one of the most common benign endometrioid proliferations, especially among premenopausal women. Although it is considered benign, endometriosis shares biological characteristics with malignant tumors, including invasion, implantation, metastasis, and recurrence. Abdominal wall endometriosis (AWE) refers to the presence of endometriosis lesions within the abdominal wall, with an extremely low incidence. Malignant transformation of AWE is exceptionally rare. CASE PRESENTATION: A 39-year-old female was admitted to the hospital on May 11, 2023, due to progressive enlargement of an abdominal mass noticed over a period of 4 months. To our knowledge, malignant transformation of abdominal wall endometriosis (AWE) is extremely rare in clinical practice, and cases of endometrioid adenocarcinoma arising from cesarean section-related AWE are even more scarce. Her medical history included surgery for a left lung teratoma 20 years ago and a cesarean section 6 years ago, with no family history of malignant tumor. This report presents a case of AWE subsequent to cesarean section, demonstrating a rare occurrence of malignant transformation into endometrioid adenocarcinoma. CONCLUSION: This article emphasizes the need for heightened vigilance regarding the possibility of malignant transformation in AWE patients and suggests a multidisciplinary team (MDT) approach and individualized treatment to improve clinical outcomes. A summary of the malignant transformation associated with endometrioid adenocarcinoma in cases of AWE has been provided to describe the Pathogenesis, Clinical Manifestation, Auxiliary Examination, Pathological Features, Treatment and Follow-up of this rare condition.
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Case

A 39-year-old female was admitted to the hospital on May 11, 2023, due to progressive enlargement of an abdominal mass noticed over a period of 4 months. Her medical history included surgery for a left lung teratoma 20 years ago and a cesarean section 6 years ago, with no family history of malignant tumors. Upon physical examination, a transverse cesarean section scar approximately 10 cm long was observed in the lower abdomen, along with a palpable, immobile, and well-defined mass in the left lower abdominal wall at a distance from the scar. Abdominal ultrasound upon admission revealed a cystic-solid mixed mass measuring 126×112 × 108 mm in lower abdomen, without blood flow signals ( Figure 1 ), however this finding may be influenced thick abdominal fat layer (BMI: 38.97kg/m 2 ). Abdominal enhanced CT scan exhibited a mass measuring 117×112 mm in anterior abdominal wall, suspected to originate from mesenchymal tissue, not ruling out leiomyoma with degeneration or sarcoma, without pelvic abdominal lymph node metastasis ( Figure 2 ). Tumor markers showed serums CA125: 20.0 U/mL, CEA: 1.07 ng/mL, CA199: 3.90 U/mL, CA153: 8.2 U/mL, SCC: 0.330 ng/mL and HE4: 361.92 pmol/L (elevated). Figure 1 Abdominal ultrasound showing a solid cystic mass in the pelvic cavity (( A ) Hyperechoic solid component and adjacent anechoic cystic region; ( B ) No blood flow signal in mass; M. solid cystic mass; Red arrow indicate solid component of the mass). Figure 2 Preoperative contrast-enhanced abdominal computed tomography (CT) scans revealing a soft tissue mass in the anterior pelvic abdominal wall. Radiological findings suggested a mesenchymal-origin lesion, with degenerative leiomyoma or sarcomatous change not ruled out. (( A ) Unenhanced axial CT scan of the pelvis; ( B ) Contrast-enhanced axial CT scan of the pelvis ( C ) Contrast-enhanced sagittal CT scan of the pelvis; Red arrows indicate the location of the mass, in the abdominal wall layer). Abdominal ultrasound showing a solid cystic mass in the pelvic cavity (( A ) Hyperechoic solid component and adjacent anechoic cystic region; ( B ) No blood flow signal in mass; M. solid cystic mass; Red arrow indicate solid component of the mass). Preoperative contrast-enhanced abdominal computed tomography (CT) scans revealing a soft tissue mass in the anterior pelvic abdominal wall. Radiological findings suggested a mesenchymal-origin lesion, with degenerative leiomyoma or sarcomatous change not ruled out. (( A ) Unenhanced axial CT scan of the pelvis; ( B ) Contrast-enhanced axial CT scan of the pelvis ( C ) Contrast-enhanced sagittal CT scan of the pelvis; Red arrows indicate the location of the mass, in the abdominal wall layer). Subsequently, on May 11, 2023, the patient underwent a combination of laparoscopic exploration, abdominal wall mass resection, and abdominal wall plastic surgery: The tumor was initially identified extraperitoneally in the lower abdomen during laparoscopy. A longitudinal incision was then made in the midline of the lower abdomen, revealing a tumor within the rectus abdominis muscle with distinct borders, solid cystic texture, and dimensions of approximately 15 cm×16 cm ( Figure 3 ). The tumor had invaded the posterior sheath and peritoneum, which were excised using an ultrasonic knife (Preoperative contrast-enhanced abdominal computed tomography (CT) scans revealing a soft tissue mass in the anterior pelvic abdominal wall. Radiological findings suggested a mesenchymal-origin lesion, with degenerative leiomyoma or sarcomatous change not ruled out. (A. Unenhanced axial CT scan of the pelvis; B. Contrast-enhanced axial CT scan of the pelvis C. Contrast-enhanced sagittal CT scan of the pelvis; Red arrows indicate the location of the mass). Following this excision, the peritoneal layer was closed, the anterior peritoneal space was freed, and a biological patch was inserted. The anterior sheath was closed, and the patch was sutured in place, with placement of a negative pressure drainage tube. Postoperative pathology revealed highly differentiated adenocarcinoma with squamous cell features, consistent with endometrioid carcinoma ( Figure 4 ). Immunohistochemistry demonstrated positive staining for CKpan (mostly+), partially positive staining for CK7, PAX-8, Vimentin and CD10, weakly positive staining for CDX-2 in focal areas and approximately 40% positive staining for Ki67. Negative staining was observed for Villin. Figure 3 Intraoperative macroscopic view of the Anterior abdominal exenteration specimen (( A ) gross specimen; ( B ) The interior of the specimen after incision; Arrows indicate old bleeding). Figure 4 Histology of Anterior abdominal exenteration specimen (endometrial glands with surrounding stromal tissues). Intraoperative macroscopic view of the Anterior abdominal exenteration specimen (( A ) gross specimen; ( B ) The interior of the specimen after incision; Arrows indicate old bleeding). Histology of Anterior abdominal exenteration specimen (endometrial glands with surrounding stromal tissues). Two weeks post-operation, the patient exhibited poor abdominal wound healing accompanied by purulent secretions. A CT examination revealed a new low-density cystic lesion beneath the skin. Wound debridement and puncture drainage were performed, leading to gradual improvement in the abdominal wound. The patient underwent three courses of adjuvant chemotherapy following surgery. Diagnostic curettage pathology indicated atypical endometrial hyperplasia. Currently, the patient’s condition is stable, hysterectomy with bilateral salpingo-oophorectomy and pelvic and abdominal lymph node dissection are recommended.

Intro

Endometriosis is defined as the presence of endometrial glands and stroma outside the uterine cavity. 1 It affects approximately 176 million women worldwide, with an incidence rate of 10–15% among women of childbearing age. 1 As a benign disease, endometriosis exhibits characteristics reminiscent of malignant tumors, 2 and a small percentage (0.7% to 1%) of endometriosis patients have a risk of malignancy. In 1925, Sampson first described of malignant transformation of ectopic endometrial tissue and proposed three diagnostic criteria for the disease: (1) close association of endometriosis with the tumor; (2) histological consistency with endometrial origin; (3) absence of other primary tumor sites. Subsequently, in 1953, Scott introduced an additional diagnostic criterion: (4) morphologic demonstration of benign endometriosis contiguous with malignant tissue. 2 , 3 However, the clinical application of these criteria has limitations, especially when dealing with small adjacent benign endometriosis lesions or those affected by adjacent malignant tissue destruction. Therefore, in clinical practice, a comprehensive diagnosis should also consider the patient’s history and clinical manifestations. It is worth noting that 80% of endometriosis-associated malignancies (EAM) manifest within the ovaries, while extrinsic EAM primarily occurs in the rectosigmoid colon and rectovaginal septum. 4 AWE refers to the presence of endometriosis lesions within the abdominal wall, with an exceedingly low incidence ranging from 0.03% to 1.34%. 4 , 5 AWE includes both primary cases (predominantly located in the umbilicus or groin) and secondary cases (resulting from trauma or surgery, particularly after cesarean section). 6 Notably, the malignant transformation of AWE is even rarer, with an incidence of 0.3% to 1.0%, and most cases are documented in case reports. 7 Malignant transformation of AWE is rare, with challenging preoperative diagnosis, limited treatment experience, and potentially poor prognosis. In this report, we present a rare case of secondary AWE (subsequent to cesarean section) that underwent malignant transformation into endometrioid adenocarcinoma, aiming to provide valuable clinical reference for the diagnosis and management of this uncommon entity.

Conclusion

We suggest the following: (1) It is crucial to implement preventive measures, such as reducing cesarean section rates and meticulous incision protection, to minimize iatrogenic endometrial implantation. (2) The assessment of abdominal wall masses requires integration of clinical and radiologic information. Biopsy and histopathology are required to confirm the diagnosis. (3) Although there is no consensus on the optimal surgical approach, for patients not desiring fertility preservation, upon confirmation of malignant transformation of AWE, abdominal wall mass resection, prophylactic hysterectomy, bilateral adnexectomy, and pelvic and abdominal lymph node dissection should be considered.

Discussion

A study by Liu et al 6 found that in 46 patients with malignant transformation of AWE, clear cell carcinoma accounted for 71.7% (33/46) of cases, followed by endometrioid carcinoma at 8.7% (4/46), serous adenocarcinoma at 6.5% (3/46), and other types at 13% (6/46). We conducted an investigation using PUBMED, combining keywords such as “carcinoma”, “adenocarcinoma”, “malignancy”, “endometriosis” and “abdominal wall scar”. The search covered literature from January 1980 to April 2024. We identified a total of seven AWE cases with pathologically confirmed endometrioid adenocarcinoma: five cases of malignant transformation confirmed as endometrioid carcinoma, one case with both endometrioid carcinoma and clear cell carcinoma, and another case combining endometrioid carcinoma and serous carcinoma ( Table 1 ). 8–14 Table 1 Case of AWE with Pathologically Confirmed Endometrioid Adenocarcinoma in the Literature Author Year Age Operation History Imaging Examination Tumor Maker (U/mL) Mass Location Mass Size Surgery and Post-Operation Treatment Pathology Other Şahin O 8 2021 44 Cesarean section PET-CT CA125 normal Cesarean scar Not provided Abdominal hysterectomy bilateral salpingo-oophorectomy systematic pelvic and para-aortic lymphadenectomy, the residual tumor in the left rectus muscle was excisedd Endometrioid adenocarcinoma grade II At a postoperative follow-up in the 4h year, no relapsed tumor or metastasis was seen on imaging. Paulino E 9 2020 45 A right hemicolectomy of a benign condition 23 years ago CT X-ray Not provided The right lower quadrant of abdomen 10×6 cm Plastic surgeon and connective tissue surgeon, decided to perform a wide resection of the abdominal wall along with hysterectomy and salpingo-oophorectomy Post-operation with megestrol acetate 160 mg/daily. The uterine specimen: a superficial endometrioid adenocarcinoma grade 1 Tsuruga T 10 2019 49 Laparoscopic ovarian endometriosis cyst resection 15 years ago Ultrasound MRI PET-CT CA125:90 CA199:222 Cannula scar 4 cm Radical margin resection of the abdominal wall tumor, flap reconstruction of the abdominal wall, hysterectomy, bilateral salpingooophorectomy and omental biopsy Systemic chemotherapy (six cycles of tri-weekly carboplatin and paclitaxel) Mixed endometrioid and clear cell carcinoma Vinchant M 11 2013 43 Two cesarean sections Last surgery 10 years ago Ultrasound MRI revealed enlargement of external iliac and right inguinal lymph nodes PET-CT Cesarean scar 13×9 cm 4 cycles of chemotherapy (Caelyx-carboplatin) followed by complete surgical resection (hysterectomy and bilateral salpingo-oophorectomy with pelvic, paraaortic and right inguinal lymphadenectomy) Endometrioid grade II BMI28.7 Peer M 12 2013 44 Open appendectomy Ultrasound MRI PET-CT CA125 normal Over the symphysis pubis 3×1.8×1.8 cm Resection of the mons pubis and the right pelvic and inguinofemoral lymph nodes Chemotherapy: One cycles of carboplatin and paclitaxel five cycles of epirubicin and carboplatin Local radiotherapy Large areas of highly differentiated endometrioid adenocarcinoma and small areas of adeno-squamous and serous-papillary differentiation Da Ines D 13 2011 48 Two cesarean sections 16 years ago, 20 years ago MRI PET-CT All normal Cesarean scar 6×5.5×4 cm Pre-operation six courses of chemotherapy (Taxolw and Carboplatinew) A laparoscopic hysterectomy with bilateral salpingo-oophorectomy and installation of abdominal wall prosthesis Mixed endometrioid and serous carcinoma No sign of recurrence 15 month Drukała Z 14 2010 43 (1997) Caesarean section 17 years age Not provided Not provided Cesarean scar Not provided Post-caesarean scar tumour was removed and a hysterectomy Papillary endometrioid adenocarcinoma in the abdominal wall tumour Recurrence in the left inguinal region was observed. The tumour with lymph nodes around left iliac vessels was excised and a mesh was sewn into the abdominal wall defect, abd the adnexa were removed bilaterally 2 months later (2001). Progression in the soft tissues of the pubic region, radical irradiation was instituted (2002). Pubic bone destruction and pressing on the urinary bladder. Nine cycles of chemotherapy of the PAC regimen (cyclophosphamide, cisplatin, doxorubicin) and onecycle of the VFP regimen (cisplatin, etoposide, 5-fluorouracil) were delivered (2006). Died of generalized neoplastic disease (2008). Case of AWE with Pathologically Confirmed Endometrioid Adenocarcinoma in the Literature Endometriosis is a complex and multifactorial benign condition, yet its pathophysiological mechanisms remain poorly understood. The main theories on the origin of ectopic endometrium include retrograde menstruation, coelomic metaplasia, lymphatic and vascular metastasis, and stem cell theory. The formation of ectopic lesions is influenced by various factors such as hormone, heredity, immunity and environment. There are two prevailing hypotheses concerning malignant transformation of endometriosis: firstly, typical endometriosis serves as a precancerous state with Endometriosis-Associated Malignancy (EAM) evolving from atypical endometriosis; secondly, endometriosis and EAM share a comparable “tissue environment”. Indeed, the coexistence of benign lesions and malignant tumor tissues in certain instances supports the latter point. Malignant transformation of AWE, particularly endometrioid adenocarcinoma, is rare, The molecular mechanism of malignant transformation of endometriosis is currently based on studies of endometriosis associated ovarian carcinoma (EAOC). Studies suggest a correlation between genetic mutations and the pathogenesis of endometriosis and EAM: (1) PTEN gene: Loss of heterozygosity (LOH) in the tumor suppressor gene PTEN , leading to the activation of the downstream PI3K/AKT/mTOR signaling pathway, is considered a significant mechanism contributing to the onset and progression of endometriosis. Sato et al 15 additionally confirmed PTEN mutation in 42.15% of endometriosis-associated ovarian endometrioid adenocarcinomas and 27.3% of endometriosis-associated ovarian clear cell carcinomas; (2) ARID1A gene: Wiegand et al 16 reported ARID1A gene mutations in 30% of endometriosis-associated ovarian endometrioid adenocarcinomas and 46% of endometriosis-associated ovarian clear cell carcinomas. Furthermore, mutations were observed in atypical endometriosis proximal to the tumor, yet absent in distant endometriosis. Therefore, ARID1A mutation is regarded as an early event in malignant transformation; (3) Changes in CTNNB1 and RAS genes also play a significant role in the malignancy of endometriosis. 2 Patients with AWE typically present with complaints of discovering nodules or masses on the abdominal wall, often accompanied by periodic or irregular pain. Among imaging methods, ultrasound is the most commonly used in clinical settings due to its convenience and cost-effectiveness. Ultrasound can visualize masses within the soft tissue layer of the abdominal wall, displaying either isoechoic or hyperechoic characteristics, while blood flow signals can be detected by color doppler ultrasonography. MRI provides high-resolution soft tissue images, enabling observation of irregular masses in the abdominal wall that extend into layers such as adipose tissue, fascia, muscle, or peritoneum. CT imaging reveals irregular masses in the abdominal wall with uneven enhancement. Additionally, CT scans can detect metastases in various regions such as the groin, pelvis, abdominal paracolic gutter, cardiophrenic angle, mediastinum, and upper and lower clavicular lymph nodes, assisting in determination the presence of distant metastasis. Elevated CA125 levels exceeding 200 U/mL are typically observed in cases of EAM, while in malignant transformation of AWE, CA125 levels are usually normal or only slightly elevated. Thus, CA125 is of limited value in diagnosing malignant transformation of AWE. Therefore, CA125 levels are not as valuable in diagnosing malignant transformation of AWE. 2 , 6 In this case, because CT scan exhibited a mass suspected to originate from mesenchymal tissue, and CA125 is normal, We did not diagnose malignant transformation of AWF preoperatively. We found that in the reported cases, puncture biopsy and histopathological examination is helpful to make a definite diagnosis. The predominant pathological pattern of EAOC is typically endometrioid adenocarcinoma. However, clear cell carcinoma is the most frequently reported type of malignant transformation of AWE. This is followed by endometrioid adenocarcinoma, serous carcinoma, and other relatively rare mixed cancers. The use of immunohistochemical staining combined with pathological features can improve the accuracy of diagnosing endometrioid adenocarcinoma. Notably, typical endometrioid morphology can be seen at low magnification, characterized by densely packed endometrioid glands with sparse interstitium. At medium magnification, columnar cells are arranged around the endometrioid glands, while at high magnification, pseudostratified nuclei exhibit no more than moderate atypia, the cytoplasm appears small, and the nuclei are oval-shaped. 17 The immunohistochemical analysis, in line with the literature’s findings, provides additional support for the diagnosis of endometrioid adenocarcinoma in this case. 18 , 19 There is no consensus on the optimal surgical and postoperative approach. However, the current common treatment for malignant transformation of AWE is wide resection. Most studiers suggest that abdominal wall tumor resection should be accompanied by hysterectomy and bilateral adnexectomy, as well as inguinal lymph node dissection. Adjuvant chemotherapy and radiotherapy are administered post-surgery in some cases, in this case three cycles of adjuvant chemotherapy were also administered. A study of 33 cases reported a high recurrence rate within 2 years and poor prognosis for malignant transformation of AWE. Specifically, 17 cases experienced recurrence or progression within 2 years, while 3 cases showed recurrence or progression after 2 years. 6

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