Single-cell analysis reveals landscape of endometrial cancer response to estrogen and identification of early diagnostic markers

Dong, Chunli; Zhao, Liyan; Liu, Xiongtao; Dang, Ling; Zhang, Xin

doi:10.1371/journal.pone.0301128

PLoS ONE

2024

DOI: 10.1371/journal.pone.0301128

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Single-cell analysis reveals landscape of endometrial cancer response to estrogen and identification of early diagnostic markers

Chunli Dong,

Liyan Zhao,

Xiongtao Liu

et al.

Abstract: Background The development of endometrial cancer (EC) is closely related to the abnormal activation of the estrogen signaling pathway. Effective diagnostic markers are important for the early detection and treatment of EC. Method We downloaded single-cell RNA sequencing (scRNA-seq) and spatial transcriptome (ST) data of EC from public databases. Enrichment scores were calculated for EC cell subpopulations using the “AddModuleScore” function and the AUCell package, respectively. Six predictive models were con… Show more

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Cited by 2 publications

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Tumor and peritumoral tissue hormonal background features in patients with rare types of endometrial cancer

Frantsiyants,

Bandovkina,

Menshenina

et al. 2024

Issled. prakt. med. (Print)

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Serous endometrial intraepithelial carcinoma (SEIC) and clear cell carcinoma of the endometrium (CCEC) belong to pathogenetic type II without evidence of hyperestrogenism, are often detected late in the course of the disease, and are characterized by an aggressive course. Currently, there is increasing interest in the role of local content and metabolism of steroid hormones in organs and tissues in various pathologies, including the development of malignant tumors. Purpose of the study. To determine the local level of sex hormones in patients with SEIC and CCEC. Patients and methods. The study included 21 patients with SEIC and 20 patients with CCEC. The control group consisted of 20 patients who had undergone surgical treatment for uterine myoma. All patients were treated at the National Medical Research Center for Oncology, Rostov‑on‑ Don, the Russian Federation Ministry of Health. The local levels of estrogens and androgens were determined in the tumor tissue, the perifocal zone, endometrial tissue unaffected by the tumor process, and the fallopian tube tissue in patients with SEIC and CCEC. In the control group, the local level of sex hormones was determined in intact 10 % homogenic endometrial tissue. Results. The data were analyzed, and the results demonstrated that the tumors and peritumoral tissues exhibited a depletion of estradiol (E2), a saturation of testosterone, and an extreme saturation of estriol (E3). The consequence of this imbalance was the predominance of fetal placental estrogen (E3), which was detected not only in the tumor tissue but also in distant parts of the endometrium and uterine tubes. In these regions, the concentration of E3 exceeded that of intact endometrium by a factor of more than five. A comparison of estrogen receptor (ER) levels revealed elevated levels in samples of the tumor, its perifocal zone, distant endometrium, and fallopian tubes. This finding indicated a predominance of ERα over ERβ. Conclusion. The local hormonal background of rare forms of non‑endometrioid endometrial carcinomas exhibits distinctive characteristics, including the replacement of the influence of classical estrogen (E2) by fetal, placental E3. Additionally, there is a notable prevalence of the REα type over REβ, along with hyperandrogenization of tissues, which culminates in the formation of a unique low‑differentiated tumor with pronounced biological aggressiveness.

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Tumor and peritumoral tissue hormonal background features in patients with rare types of endometrial cancer

Frantsiyants,

Bandovkina,

Menshenina

et al. 2024

Issled. prakt. med. (Print)

View full text Add to dashboard Cite

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Single-cell RNA sequencing in endometrial cancer: exploring the epithelial cells and the microenvironment landscape

González-Martínez,

Pérez-Mies,

Cortés

et al. 2024

Front. Immunol.

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Single-cell RNA sequencing (scRNA-seq) technology has emerged as a powerful tool for dissecting cellular heterogeneity and understanding the intricate biology of diseases, including cancer. Endometrial cancer (EC) stands out as the most prevalent gynecological malignancy in Europe and the second most diagnosed worldwide, yet its cellular complexity remains poorly understood. In this review, we explore the contributions of scRNA-seq studies to shed light on the tumor cells and cellular landscape of EC. We discuss the diverse tumoral and microenvironmental populations identified through scRNA-seq, highlighting the implications for understanding disease progression. Furthermore, we address potential limitations inherent in scRNA-seq studies, such as technical biases and sample size constraints, emphasizing the need for larger-scale research encompassing a broader spectrum of EC histological subtypes. Notably, a significant proportion of scRNA-seq analyses have focused on primary endometrioid carcinoma tumors, underscoring the need to incorporate additional histological and aggressive types to comprehensively capture the heterogeneity of EC. By critically evaluating the current state of scRNA-seq research in EC, this review underscores the importance of advancing towards more comprehensive studies to accelerate our understanding of this complex disease.

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Single-cell analysis reveals landscape of endometrial cancer response to estrogen and identification of early diagnostic markers

Cited by 2 publications

References 61 publications

Tumor and peritumoral tissue hormonal background features in patients with rare types of endometrial cancer

Tumor and peritumoral tissue hormonal background features in patients with rare types of endometrial cancer

Single-cell RNA sequencing in endometrial cancer: exploring the epithelial cells and the microenvironment landscape

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