Your search keyword '"Germ cell neoplasia in situ"' showing total 91 results

1. Cellular Senescence in Germ Cell Neoplasia In Situ (GCNIS) and Other Histological Types of Testicular Cancer.

Author

Tatanis, Vasileios, Veroutis, Dimitris, Pantelis, Pavlos, Theocharous, George, Sarlanis, Helen, Georgiou, Alexandros, Mulita, Francesk, Peteinaris, Angelis, Natsos, Anastasios, Moulavasilis, Napoleon, Kavantzas, Nikolaos, Kotsinas, Athanassios, and Adamakis, Ioannis

Subjects

CELLULAR aging, TESTICULAR cancer, GERM cells, TUMORS, PRECANCEROUS conditions, IMMUNOSENESCENCE, TESTIS surgery, ORCHIOPEXY, AGING

Abstract

Background and Objectives: The presence and contribution of senescent cells in premalignant lesions is well documented, but not in germ cell neoplasia in situ. The purpose of this study is to identify the presence of senescent cells in pre-malignant testicular conditions and in different histological types of testicular cancer. Materials and Methods: Thirty patients who underwent orchiectomy due to testicular tumors were included. Formalin-fixed paraffin-embedded (FFPE) testicular tissue for each patient was available. Sections from these specimens were examined by immunohistochemical analysis with the following markers: GL13 for cellular senescence, p21WAF1/Cip1 for cell cycle arrest, and Ki67 for cell proliferation. Results: Thirteen (43.3%) suffered from seminoma with a mean total proportion of GCNIS senescence of 20.81 ± 6.81%. In the group of embryonal testicular tumors, nine (30%) patients were included, with an average rate of 6.64 ± 5.42% of senescent cells in GCNIS. One (3.3%) patient suffered from chondrosarcoma in which 7.9% of GL13+ cells were detected in GCNIS. Four (13.4%) patients suffered from teratoma and three (10%) from yolk sac tumors, while GCNIS senescence was detected in a range of 4.43 ± 1.78% and 3.76 ± 1.37%, respectively. Conclusions: Cellular senescence was detected in both germ cell neoplasia in situ and testicular cancer, but was more prevalent within the premalignant lesions. [ABSTRACT FROM AUTHOR]

Published

2024

2. Cellular Senescence in Germ Cell Neoplasia In Situ (GCNIS) and Other Histological Types of Testicular Cancer

Author

Vasileios Tatanis, Dimitris Veroutis, Pavlos Pantelis, George Theocharous, Helen Sarlanis, Alexandros Georgiou, Francesk Mulita, Angelis Peteinaris, Anastasios Natsos, Napoleon Moulavasilis, Nikolaos Kavantzas, Athanassios Kotsinas, and Ioannis Adamakis

Subjects

germ cell neoplasia in situ, GL13, immunohistochemistry, senescence, testicular cancer, Medicine (General), R5-920

Abstract

Background and Objectives: The presence and contribution of senescent cells in premalignant lesions is well documented, but not in germ cell neoplasia in situ. The purpose of this study is to identify the presence of senescent cells in pre-malignant testicular conditions and in different histological types of testicular cancer. Materials and Methods: Thirty patients who underwent orchiectomy due to testicular tumors were included. Formalin-fixed paraffin-embedded (FFPE) testicular tissue for each patient was available. Sections from these specimens were examined by immunohistochemical analysis with the following markers: GL13 for cellular senescence, p21WAF1/Cip1 for cell cycle arrest, and Ki67 for cell proliferation. Results: Thirteen (43.3%) suffered from seminoma with a mean total proportion of GCNIS senescence of 20.81 ± 6.81%. In the group of embryonal testicular tumors, nine (30%) patients were included, with an average rate of 6.64 ± 5.42% of senescent cells in GCNIS. One (3.3%) patient suffered from chondrosarcoma in which 7.9% of GL13+ cells were detected in GCNIS. Four (13.4%) patients suffered from teratoma and three (10%) from yolk sac tumors, while GCNIS senescence was detected in a range of 4.43 ± 1.78% and 3.76 ± 1.37%, respectively. Conclusions: Cellular senescence was detected in both germ cell neoplasia in situ and testicular cancer, but was more prevalent within the premalignant lesions.

Published

2024

3. Dysgenetic Gonads

Author

Newbould, Melanie Joy, Singh, Naveena, Series Editor, McCluggage, W. Glenn, Series Editor, and Wilkinson, Nafisa, editor

Published

2023

4. The Role of miRNA in Testicular Cancer: Current Insights and Future Perspectives.

Author

Ditonno, Francesco, Franco, Antonio, Manfredi, Celeste, Fasanella, Daniela, Abate, Marco, La Rocca, Roberto, Crocerossa, Fabio, Iossa, Vincenzo, Falagario, Ugo Giovanni, Cirillo, Luigi, Altieri, Vincenzo Maria, Di Mauro, Ernesto, Crocetto, Felice, Barone, Biagio, Cilio, Simone, Pandolfo, Savio Domenico, Aveta, Achille, Mirone, Vincenzo, Franzese, Corrado Aniello, and Arcaniolo, Davide

Subjects

MICRORNA, NON-coding RNA, TUMOR markers, CANCER chemotherapy, EARLY diagnosis, TESTICULAR cancer

Abstract

Background and Objectives: Despite advancements in the diagnosis and treatment of testicular germ cell tumours (TGTCs), challenges persist in identifying reliable biomarkers for early detection and precise disease management. This narrative review addresses the role of microRNAs (miRNAs) as potential diagnostic tools and therapeutic targets in the treatment of TGCTs. Materials and Methods: Three databases (PubMed®, Web of Science™, and Scopus®) were queried for studies investigating the utility of miRNA as diagnostic tools, assessing their prognostic significance, and evaluating their potential to guide TGCT treatment. Different combinations of the following keywords were used, according to a free-text protocol: "miRNA", "non-coding RNA", "small RNA", "Testicular Cancer", "seminomatous testicular germ cell", "non-seminomatous testicular germ cell". Results: The potential of miRNAs as possible biomarkers for a non-invasive diagnosis of TGCT is appealing. Their integration into the diagnostic pathway for TGCT patients holds the potential to enhance the discriminative power of conventional serum tumour markers (STMs) and could expedite early diagnosis, given that miRNA overexpression was observed in 50% of GCNIS cases. Among miRNAs, miR-371a-3p stands out with the most promising evidence, suggesting its relevance in the primary diagnosis of TGCT, particularly when conventional STMs offer limited value. Indeed, it demonstrated high specificity (90–99%) and sensitivity (84–89%), with good positive predictive value (97.2%) and negative predictive value (82.7%). Furthermore, a direct relationship between miRNA concentration, disease burden, and treatment response exists, regardless of disease stages. The initial evidence of miRNA decrease in response to surgical treatment and systemic chemotherapy has been further supported by more recent results suggesting the potential utility of this tool not only in evaluating treatment response but also in monitoring residual disease and predicting disease relapse. Conclusions: MiRNAs could represent a reliable tool for accurate diagnosis and disease monitoring in the treatment of TGCT, providing more precise tools for early detection and treatment stratification. Nevertheless, well-designed clinical trials and comprehensive long-term data are needed to ensure their translation into effective clinical tools. [ABSTRACT FROM AUTHOR]

Published

2023

5. Male Infertility and the Risk of Developing Testicular Cancer: A Critical Contemporary Literature Review.

Author

Maiolino, Giuseppe, Fernández-Pascual, Esaú, Ochoa Arvizo, Mario Alberto, Vishwakarma, Ranjit, and Martínez-Salamanca, Juan Ignacio

Subjects

TESTICULAR cancer, MALE infertility, LITERATURE reviews, GERM cells, SPERM count, INFERTILITY, DYSGENESIS

Abstract

Background and Objectives: The relationship between male infertility (MI) and testicular cancer (TC) is bilateral. On one hand, it is well-established that patients diagnosed with TC have a high risk of pre- and post-treatment infertility. On the other hand, the risk of developing TC in male infertile patients is not clearly defined. The objective of this review is to analyze the histopathological, etiological, and epidemiological associations between MI and the risk of developing testicular cancer. This review aims to provide further insights and offer a guide for assessing the risk factors for TC in infertile men. Materials and Methods: A comprehensive literature search was conducted to identify relevant studies discussing the relationship between MI and the risk of developing TC. Results: The incidence rates of germ cell neoplasia in situ (GCNIS) appear to be high in infertile men, particularly in those with low sperm counts. Most epidemiological studies have found a statistically significant risk of developing TC among infertile men compared to the general or fertile male populations. The concept of Testicular Dysgenesis Syndrome provides an explanatory model for the common etiology of MI, TC, cryptorchidism, and hypospadias. Clinical findings such as a history of cryptorchidism could increase the risk of developing TC in infertile men. Scrotal ultrasound evaluation for testis lesions and microlithiasis is important in infertile men. Sperm analysis parameters can be useful in assessing the risk of TC among infertile men. In the future, sperm and serum microRNAs (miRNAs) may be utilized for the non-invasive early diagnosis of TC and GCNIS in infertile men. Conclusions: MI is indeed a risk factor for developing testicular cancer, as demonstrated by various studies. All infertile men should undergo a risk assessment using clinical examination, ultrasound, and semen parameters to evaluate their risk of TC. [ABSTRACT FROM AUTHOR]

Published

2023

6. Testis and Paratesticular Tissues

Author

Wilkerson, Myra L., Cheng, Liang, Lin, Fan, editor, Prichard, Jeffrey W., editor, Liu, Haiyan, editor, and Wilkerson, Myra L., editor

Published

2022

7. The Role of miRNA in Testicular Cancer: Current Insights and Future Perspectives

Author

Francesco Ditonno, Antonio Franco, Celeste Manfredi, Daniela Fasanella, Marco Abate, Roberto La Rocca, Fabio Crocerossa, Vincenzo Iossa, Ugo Giovanni Falagario, Luigi Cirillo, Vincenzo Maria Altieri, Ernesto Di Mauro, Felice Crocetto, Biagio Barone, Simone Cilio, Savio Domenico Pandolfo, Achille Aveta, Vincenzo Mirone, Corrado Aniello Franzese, Davide Arcaniolo, and Luigi Napolitano

Subjects

biomarker, germ cell neoplasia in situ, germ cell tumour, microRNA, Medicine (General), R5-920

Abstract

Background and Objectives: Despite advancements in the diagnosis and treatment of testicular germ cell tumours (TGTCs), challenges persist in identifying reliable biomarkers for early detection and precise disease management. This narrative review addresses the role of microRNAs (miRNAs) as potential diagnostic tools and therapeutic targets in the treatment of TGCTs. Materials and Methods: Three databases (PubMed®, Web of Science™, and Scopus®) were queried for studies investigating the utility of miRNA as diagnostic tools, assessing their prognostic significance, and evaluating their potential to guide TGCT treatment. Different combinations of the following keywords were used, according to a free-text protocol: “miRNA”, “non-coding RNA”, “small RNA”, “Testicular Cancer”, “seminomatous testicular germ cell”, “non-seminomatous testicular germ cell”. Results: The potential of miRNAs as possible biomarkers for a non-invasive diagnosis of TGCT is appealing. Their integration into the diagnostic pathway for TGCT patients holds the potential to enhance the discriminative power of conventional serum tumour markers (STMs) and could expedite early diagnosis, given that miRNA overexpression was observed in 50% of GCNIS cases. Among miRNAs, miR-371a-3p stands out with the most promising evidence, suggesting its relevance in the primary diagnosis of TGCT, particularly when conventional STMs offer limited value. Indeed, it demonstrated high specificity (90–99%) and sensitivity (84–89%), with good positive predictive value (97.2%) and negative predictive value (82.7%). Furthermore, a direct relationship between miRNA concentration, disease burden, and treatment response exists, regardless of disease stages. The initial evidence of miRNA decrease in response to surgical treatment and systemic chemotherapy has been further supported by more recent results suggesting the potential utility of this tool not only in evaluating treatment response but also in monitoring residual disease and predicting disease relapse. Conclusions: MiRNAs could represent a reliable tool for accurate diagnosis and disease monitoring in the treatment of TGCT, providing more precise tools for early detection and treatment stratification. Nevertheless, well-designed clinical trials and comprehensive long-term data are needed to ensure their translation into effective clinical tools.

Published

2023

8. Testis and Paratesticular Lesions

Author

Zynger, Debra L., Guo, Charles C., Lin, Fan, Series Editor, Yang, Ximing J., Series Editor, and Zhou, Ming, editor

Published

2021

9. Cancer Stem Cell Niche and Immune-Active Tumor Microenvironment in Testicular Germ Cell Tumors

Author

Kalavska, Katarina, Kucerova, Lucia, Schmidtova, Silvia, Chovanec, Michal, Mego, Michal, Crusio, Wim E., Series Editor, Lambris, John D., Series Editor, Radeke, Heinfried H., Series Editor, Rezaei, Nima, Series Editor, and Birbrair, Alexander, editor

Published

2020

10. Germ Cell Tumors Derived from Germ Cell Neoplasia In Situ

Author

Nistal, Manuel, González-Peramato, Pilar, Nistal, Manuel, and González-Peramato, Pilar

Published

2020

11. Male Infertility and the Risk of Developing Testicular Cancer: A Critical Contemporary Literature Review

Author

Giuseppe Maiolino, Esaú Fernández-Pascual, Mario Alberto Ochoa Arvizo, Ranjit Vishwakarma, and Juan Ignacio Martínez-Salamanca

Subjects

male infertility, testicular cancer, risk factors, germ cell neoplasia in situ, scrotal ultrasound, Medicine (General), R5-920

Abstract

Background and Objectives: The relationship between male infertility (MI) and testicular cancer (TC) is bilateral. On one hand, it is well-established that patients diagnosed with TC have a high risk of pre- and post-treatment infertility. On the other hand, the risk of developing TC in male infertile patients is not clearly defined. The objective of this review is to analyze the histopathological, etiological, and epidemiological associations between MI and the risk of developing testicular cancer. This review aims to provide further insights and offer a guide for assessing the risk factors for TC in infertile men. Materials and Methods: A comprehensive literature search was conducted to identify relevant studies discussing the relationship between MI and the risk of developing TC. Results: The incidence rates of germ cell neoplasia in situ (GCNIS) appear to be high in infertile men, particularly in those with low sperm counts. Most epidemiological studies have found a statistically significant risk of developing TC among infertile men compared to the general or fertile male populations. The concept of Testicular Dysgenesis Syndrome provides an explanatory model for the common etiology of MI, TC, cryptorchidism, and hypospadias. Clinical findings such as a history of cryptorchidism could increase the risk of developing TC in infertile men. Scrotal ultrasound evaluation for testis lesions and microlithiasis is important in infertile men. Sperm analysis parameters can be useful in assessing the risk of TC among infertile men. In the future, sperm and serum microRNAs (miRNAs) may be utilized for the non-invasive early diagnosis of TC and GCNIS in infertile men. Conclusions: MI is indeed a risk factor for developing testicular cancer, as demonstrated by various studies. All infertile men should undergo a risk assessment using clinical examination, ultrasound, and semen parameters to evaluate their risk of TC.

Published

2023

12. On the origin of germ cell neoplasia in situ: Dedifferentiation of human adult Sertoli cells in cross talk with seminoma cells in vitro

Author

Cornelia Fink, Nelli Baal, Jochen Wilhelm, Poonam Sarode, Roswitha Weigel, Valérie Schumacher, Daniel Nettersheim, Hubert Schorle, Carmen Schröck, Martin Bergmann, Sabine Kliesch, Monika Kressin, and Rajkumar Savai

Subjects

Germ cell neoplasia in situ, Sertoli cell dedifferentiation, TCam-2 seminoma cell line, Coculture model, Microenvironment, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Germ cell neoplasia in situ (GCNIS) is the noninvasive precursor of testicular germ cell tumors type II, the most common cancer in young men, which originates from embryonic germ cells blocked in their maturation. GCNIS is associated with impaired Sertoli cells (SCs) that express fetal keratin 18 (KRT18) and the pluripotency factor SRY-Box transcription factor 2 (SOX2). According to the current theory concerning the origin of GCNIS, these SCs are prepubertal cells arrested in their maturation due to (epi)genetic anomalies and/or environmental antiandrogens. Thus, they are unable to support the development of germ cells, which leads to their maturational block and further progresses into GCNIS. Alternatively, these SCs are hypothesized to be adult cells dedifferentiating secondarily under the influence of GCNIS. To examine whether tumor cells can dedifferentiate SCs, we established a coculture model of adult human SCs (FS1) and a seminoma cell line similar to GCNIS (TCam-2). After 2 wk of coculture, FS1 cells showed progressive expression of KRT18 and SOX2, mimicking the in vivo changes. TCam-2 cells showed SOX2 expression and upregulation of further pluripotency- and reprogramming-associated genes, suggesting a seminoma to embryonal carcinoma transition. Thus, our FS1/TCam-2 coculture model is a valuable tool for investigating interactions between SCs and seminoma cells. Our immunohistochemical and ultrastructural studies of human testicular biopsies with varying degrees of GCNIS compared to biopsies from fetuses, patients with androgen insensitivity syndrome, and patients showing normal spermatogenesis further suggest that GCNIS-associated SCs represent adult cells undergoing progressive dedifferentiation.

Published

2021

13. Germ Cell Neoplasia In Situ

Author

Colecchia, Maurizio, Massa, Simona, van Krieken, J. H. J. M., Series Editor, Raspollini, Maria Rosaria, editor, and Lopez-Beltran, Antonio, editor

Published

2020

14. Immunohistochemical Expression of Preferentially Expressed Antigen in Melanoma (PRAME) in the Uninvolved Background Testis, Germ Cell Neoplasia In Situ, and Germ Cell Tumors of the Testis.

Author

Ricci, Costantino, Franceschini, Tania, Giunchi, Francesca, Grillini, Marco, Ambrosi, Francesca, Massari, Francesco, Mollica, Veronica, Colecchia, Maurizio, and Fiorentino, Michelangelo

Subjects

*GERM cell tumors, *TESTIS tumors, *GERM cells, *SEMINOMA, *TUMORS, *GONADS, *GERMINOMA, *TESTIS, *MELANOMA, *RETROSPECTIVE studies, *TUMOR antigens

Abstract

Objectives: Preferentially expressed antigen in melanoma (PRAME) has a key role in regulating pluripotency of primordial germ cells and in the development of germ cell tumors of the testis (GCTT). However, its immunohistochemical expression in normal testes and its neoplastic counterpart remain largely unknown.Methods: We retrospectively investigated the expression of PRAME in 26 cases of GCTT, 21 cases of germ cell neoplasia in situ (GCNIS), and 17 cases of uninvolved background testes.Results: We found that PRAME was expressed more strongly by seminomatous rather than nonseminomatous GCTT (P = .000) and by pure seminoma rather than the seminoma component of seminomatous/nonseminomatous GCTT (P = .025). In addition, GCNIS and uninvolved background testes displayed high levels of PRAME expression.Conclusions: PRAME is an additional marker for the differential diagnosis of GCTT and could play a key role in the transition from seminomatous to nonseminomatous GCTT. [ABSTRACT FROM AUTHOR]

Published

2022

15. Case report. Kiemcelneoplasie in situ in een monotestis hoeft niet direct behandeld te worden.

Author

Mathijssen, Ruud J. G., Nijs, Jelle J. G., D'Hauwers, Kathleen W. M., and de Jongh, Rik

Subjects

*GERM cells, *TESTIS, *TUMORS

Abstract

This case report describes a 32-year-old man with germ cell neoplasia in situ (GCNIS) after partial orchidectomy and contralateral orchidectomy because of a mixed germ cell tumor. The treatment of GCNIS in a solitary testis consists of radiotherapy, orchidectomy or surveillance. When choosing a treatment, it is important to take into account the desire to have children, the hormonal status, the risk of developing (recurrent) testicular cancer and the advantages and disadvantages of each treatment. This case shows that surveillance in case of an active desire to have children is safe in the short term and can have advantages over radiotherapy. In retrospect, when there is suspicion for bilateral testicular cancer, consultation with an Academic Testis Expertise Centre and cryosemen preservation is recommended when there is a desire to have children. [ABSTRACT FROM AUTHOR]

Published

2022

16. Primary Testicular Neuroendocrine Tumor Coexisting With Seminoma Sharing Germ Cell Origin.

Author

Iida, Noriyuki, Takemura, Kosuke, Ito, Masaya, Funata, Nobuaki, Yonese, Ichiro, Suzuki, Hiroaki, Tsuzuki, Toyonori, and Koga, Fumitaka

Subjects

*TERATOCARCINOMA, *NEUROENDOCRINE tumors, *SEMINOMA, *GERM cells, *FLUORESCENCE in situ hybridization, *TESTICULAR cancer

Abstract

A 40-year-old, male, Japanese patient presented with the complaint of painless, right testicular swelling. Tumor markers for testicular cancer were normal. He underwent radical orchiectomy with the clinical diagnosis of stage I seminoma. Pathological examination revealed seminoma and coexisting neuroendocrine tumor (NET). Germ cell neoplasia in situ (GCNIS) was present in the vicinity of seminoma, but there was no continuity between NET and seminoma. Tumor cells of both lesions displayed amplification of 12p and isochromosome 12p on fluorescence in situ hybridization, suggesting that both tumors originated from GCNIS. The present report is the first to describe a case of primary testicular NET coexisting with seminoma in an ipsilateral testis. [ABSTRACT FROM AUTHOR]

Published

2021

17. On the origin of germ cell neoplasia in situ: Dedifferentiation of human adult Sertoli cells in cross talk with seminoma cells in vitro.

Author

Fink, Cornelia, Baal, Nelli, Wilhelm, Jochen, Sarode, Poonam, Weigel, Roswitha, Schumacher, Valérie, Nettersheim, Daniel, Schorle, Hubert, Schröck, Carmen, Bergmann, Martin, Kliesch, Sabine, Kressin, Monika, and Savai, Rajkumar

Subjects

*SERTOLI cells, *GERM cells, *ANDROGEN receptors, *ADULTS, *TESTICULAR cancer, *SEMINOMA, *GERM cell tumors, *ANDROGEN-insensitivity syndrome

Abstract

Germ cell neoplasia in situ (GCNIS) is the noninvasive precursor of testicular germ cell tumors type II, the most common cancer in young men, which originates from embryonic germ cells blocked in their maturation. GCNIS is associated with impaired Sertoli cells (SCs) that express fetal keratin 18 (KRT18) and the pluripotency factor SRY-Box transcription factor 2 (SOX2). According to the current theory concerning the origin of GCNIS, these SCs are prepubertal cells arrested in their maturation due to (epi)genetic anomalies and/or environmental antiandrogens. Thus, they are unable to support the development of germ cells, which leads to their maturational block and further progresses into GCNIS. Alternatively, these SCs are hypothesized to be adult cells dedifferentiating secondarily under the influence of GCNIS. To examine whether tumor cells can dedifferentiate SCs, we established a coculture model of adult human SCs (FS1) and a seminoma cell line similar to GCNIS (TCam-2). After 2 wk of coculture, FS1 cells showed progressive expression of KRT18 and SOX2, mimicking the in vivo changes. TCam-2 cells showed SOX2 expression and upregulation of further pluripotency- and reprogramming-associated genes, suggesting a seminoma to embryonal carcinoma transition. Thus, our FS1/TCam-2 coculture model is a valuable tool for investigating interactions between SCs and seminoma cells. Our immunohistochemical and ultrastructural studies of human testicular biopsies with varying degrees of GCNIS compared to biopsies from fetuses, patients with androgen insensitivity syndrome, and patients showing normal spermatogenesis further suggest that GCNIS-associated SCs represent adult cells undergoing progressive dedifferentiation. [ABSTRACT FROM AUTHOR]

Published

2021

18. Histopathological Evaluation of Testicular Biopsy

Author

Meyts, Ewa Rajpert-De, Grigor, Kenneth M., Skakkebaek, Niels E., Lenzi, Andrea, Series editor, Jannini, Emmanuele A., Series editor, Simoni, Manuela, editor, and Huhtaniemi, Ilpo T., editor

Published

2017

19. Testicular Germ Cell Tumors

Author

Jimenez, Rafael E., Gupta, Sounak, Herrera-Hernandez, Loren P., Sebo, Thomas J., Nogales, Francisco F., editor, and Jimenez, Rafael E., editor

Published

2017

20. Testicular Germ Cell Tumors and Teratomas

Author

Lanza, Denise G., Heaney, Jason D., Oatley, Jon M., editor, and Griswold, Michael D., editor

Published

2017

21. Metachronous bilateral testicular cancer: Case reports and review of literature.

Author

Low, Zhi-Yang, Yan, Angela, Arul, Dhili, and Chitale, Sudhanshu

Subjects

*LITERATURE reviews, *GERM cells, *CANCER radiotherapy, *DISEASE risk factors, *TESTIS, *TESTICULAR cancer

Abstract

Background: It is well recognised that men with unilateral testicular cancer may go on to develop metachronous cancer in the contralateral testis. Here, we present two cases of metachronous bilateral testicular cancer and a literature review. Clinical cases: In both cases, the second testicular cancer occurred several years after the initial cancer, and both cases were not screened for presence of contralateral germ cell neoplasia in situ upon the first diagnosis. Discussion: We also present a literature review on the need for screening biopsies of contralateral testis for germ cell neoplasia in situ and the risk factors which should encourage screening. Furthermore, we also explore the effect of chemotherapy on the incidence of contralateral testicular cancer and the effectiveness of radiotherapy in the treatment of germ cell neoplasia in situ. Conclusion: We believe that screening biopsies of the contralateral testis upon diagnosis of unilateral testicular cancer should be encouraged as it can lead to better management of the condition and a relatively favourable outcome on functional fronts. [ABSTRACT FROM AUTHOR]

Published

2019

22. Intratubular Teratoma: A Rare Form of Testicular Germ Cell Neoplasia.

Author

Genco, Iskender Sinan, Ratzon, Fanni, Glickman, Leonard, Santagada, Eugene, and Unger, Pamela

Subjects

*GERM cell tumors, *TERATOMA, *TESTIS tumors, *EPIBLAST, *SEMINOMA, *GERM cells

Abstract

Germ cell neoplasia in situ is the initial manifestation for invasive germ cell tumor. Further progression will result in intratubular germ cell tumor with the majority being intratubular seminoma or intratubular embryonal carcinoma. Intratubular teratoma in the testis is exceptionally rare with no well-documented cases to our knowledge. In this article, we report a case of an intratubular teratoma adjacent to mixed germ cell tumor in the testis. The patient is a 34-year-old male who presented with a palpable right testicular mass and underwent right radical orchiectomy. Gross examination of the testis revealed 2.0-cm tan, well-circumscribed, firm, and nodular mass at the inferior pole. Microscopic examination revealed a mixed germ cell tumor, predominantly seminoma (95%) with embryonal carcinoma (4%) and teratoma (1%). There is also germ cell neoplasia in situ, intratubular seminoma, and intratubular teratoma at the periphery of the tumor. Tubules with intratubular teratoma were filled by neoplastic squamous cells with a single layer of germ cell neoplasia in situ at the periphery. Adjacent to the intratubular teratoma was seminoma, embryonal carcinoma, and invasive teratoma. Immunohistochemical stains showed the neoplastic squamous cells in the tubule to be positive for p40 and negative for OCT34 and D2-40. The single layer of germ cell neoplasia in situ at the periphery of the intratubular teratoma was negative for p40 and positive for OCT34 and D2-40. Although teratoma is a common component in an adult germ cell tumor, an intratubular manifestation is exceptional. The present case illustrates this rare finding. [ABSTRACT FROM AUTHOR]

Published

2019

23. Assessment of piRNA biogenesis and function in testicular germ cell tumors and their precursor germ cell neoplasia in situ.

Author

Gainetdinov, Ildar V., Skvortsova, Yulia V., Kondratieva, Sofia A., Klimov, Alexey, Tryakin, Alexey A., and Azhikina, Tatyana L.

Subjects

*TESTICULAR cancer, *GERM cell tumors, *GENETIC overexpression, *NON-coding RNA, *GENETIC regulation, *CARRIER proteins, *COMPARATIVE studies, *GENES, *GERM cells, *RESEARCH methodology, *MEDICAL cooperation, *PROTEINS, *RESEARCH, *RESEARCH funding, *RNA, *TESTIS, *TESTIS tumors, *TUMORS, *EVALUATION research, *SEQUENCE analysis

Abstract

Background: Aberrant overexpression of PIWI/piRNA pathway proteins is shown for many types of tumors. Interestingly, these proteins are downregulated in testicular germ cell tumors (TGCTs) compared to normal testis tissues. Here, we used germline and TGCT markers to assess the piRNA biogenesis and function in TGCTs and their precursor germ cell neoplasia in situ (GCNIS).Methods: We used small RNA deep sequencing, qRT-PCR, and mining public RNAseq/small RNA-seq datasets to examine PIWI/piRNA gene expression and piRNA biogenesis at four stages of TGCT development: (i) germ cells in healthy testis tissues, (ii) germ cells in testis tissues adjacent to TGCTs, (iii) GCNIS cells and (iv) TGCT cells. To this end, we studied three types of samples: (a) healthy testis, (b) testis tissues adjacent to two types of TGCTs (seminomas and nonseminomas) and containing both germ cells and GCNIS cells, as well as (c) matching TGCT samples.Results: Based on our analyses of small RNA-seq data as well as the presence/absence of expression correlation between PIWI/piRNA pathway genes and germline or TGCT markers, we can suggest that piRNA biogenesis is intact in germ cells present in healthy adult testes, and adjacent to TGCTs. Conversely, GCNIS and TGCT cells were found to lack PIWI/piRNA pathway gene expression and germline-like piRNA biogenesis. However, using an in vitro cell line model, we revealed a possible role for a short PIWIL2/HILI isoform expressed in TGCTs in posttranscriptional regulation of the youngest members of LINE and SINE classes of transposable elements. Importantly, this regulation is also implemented without involvement of germline-like biogenesis of piRNAs.Conclusions: Though further studies are warranted, these findings suggest that the conventional germline-like PIWI/piRNA pathway is lost in transition from germ cells to GCNIS cells. [ABSTRACT FROM AUTHOR]

Published

2018

24. Is the FSHR 2039A>G variant associated with susceptibility to testicular germ cell cancer?

Author

Bang, A. K., Busch, A. S., Almstrup, K., Gromoll, J., Kliesch, S., Rajpert‐De Meyts, E., Skakkebæk, N. E., Juul, A., Tüttelmann, F., and Jørgensen, N.

Subjects

*TERATOCARCINOMA, *TESTICULAR cancer, *FOLLICLE-stimulating hormone, *SINGLE nucleotide polymorphisms, *MALE infertility, *CONTROL groups

Abstract

Testicular germ cell cancer ( TGCC) is derived from germ cell neoplasia in situ ( GCNIS), which arises due to niche disturbances affecting the Sertoli cells. It is believed that exogenous endocrine factors have a crucial role in governing neoplastic transformation but on a strong hereditary background. Follicle-stimulating hormone ( FSH) is the major regulatory hormone of the Sertoli cells. FSH signalling-related single-nucleotide polymorphisms ( SNPs) have previously been shown to affect FSH action in men at different levels. We aimed to investigate whether three FSH-related SNPs ( FSHR 2039A>G, FSHR -29G>A and FSHB -211G>T) are associated with development of TGCC. A total of 752 Danish and German patients with TGCC from two tertiary andrological referral centres were included. Three control groups comprising 2020 men from the general population, 679 fertile men and 417 infertile men, were also included. Chi-squared test was performed to compare genotype- and allele frequencies. Kruskal-Wallis test was performed to compare age at diagnosis. Patients with TGCC had a higher frequency of the A-allele of FSHR 2039A>G compared to the group of fertile men with an AA-genotype frequency of 30.2% vs. 22.0%, respectively, p = 0.002. This variant is associated with higher FSH receptor activity. The distribution of the FSHR 2039A>G did not differ significantly between the patients with TGCC and the infertile or the general population. The frequency of the two other SNPs did not differ between patient with TGCC and any of the control groups. No differences were detected between genotypes and age distribution or histological subtype of the tumours. In conclusion, we observed that a genetic variant associated with FSHR activity may modulate the susceptibility to TGCC. [ABSTRACT FROM AUTHOR]

Published

2018

25. Malignant testicular germ cell tumors in postpubertal individuals with androgen insensitivity: prevalence, pathology and relevance of single nucleotide polymorphism-based susceptibility profiling.

Author

Cools, M., Wolffenbuttel, K. P., Hersmus, R., Mendonca, B. B., Kaprová, J., Drop, S. L. S., Stoop, H., Gillis, A. J. M., Oosterhuis, J. W., Costa, E. M. F., Domenice, S., Nishi, M. Y., Wunsch, L., Quigley, C. A., T'Sjoen, G., and Looijenga, L. H. J.

Subjects

*GERM cell tumors, *ANDROGENS, *SINGLE nucleotide polymorphisms, *GENETICS, *CASTRATION

Abstract

Study Question: What is the prevalence of malignant testicular germ cell tumors (TGCT) and its precursors, (pre-) germ cell neoplasia in situ (GCNIS), in late teenagers and adults who have androgen insensitivity syndrome (AIS) and the impact of an individual's genetic susceptibility to development of TGCT?Summary Answer: No GCNIS or TGCT was diagnosed, but pre-GCNIS was identified in 14 and 10% of complete and partial AIS patients, respectively, and was associated with a higher genetic susceptibility score (GSS), with special attention for KITLG (rs995030) and ATFZIP (rs2900333).What Is Known Already: Many adult women with AIS decline prophylactic gonadectomy, while data regarding the incidence, pathophysiology and outcomes of TGCT in postpubertal individuals with AIS are lacking. The relevance of genetic factors, such as single nucleotide polymorphisms (SNPs), in predisposing AIS individuals to TGCT is unknown.Study Design, Size, Duration: This multicenter collaborative study on prophylactically removed gonadal tissue was conducted in a pathology lab specialized in germ cell tumor biology.Participants/materials, Setting, Methods: Material from 52 postpubertal individuals with molecularly confirmed AIS (97 gonadal samples) was included; the median age at surgery was 17.5 (14-54) years. Immunohistochemical studies and high-throughput profiling of 14 TGCT-associated SNPs were performed. The main outcome measures were the prevalence of pre-GCNIS, GCNIS and TGCT, and its correlation with a GSS, developed based on the results of recent genome-wide association studies.Main Results and Role Of Chance: The earliest recognizable change preceding GCNIS, referred to as pre-GCNIS, was present in 14% of individuals with complete and 10% of those with partial AIS at a median age of 16 years. No GCNIS or invasive TGCT were found. The median GSS was significantly greater for those with, compared to those without, pre-GCNIS (P = 0.01), with an overlap between groups. Our data suggest important roles for risk alleles G at KITLG (rs995030) and C at ATFZIP (rs2900333), among the 14 studied TGCT-associated SNPs.Large Scale Data: N/A.Limitations Reasons For Caution: A limited number of cases were included.Wider Implications Of the Findings: Our data suggest that the prevalence of pre-GCNIS in individuals with AIS beyond puberty is around 15%. Genetic susceptibility likely contributes to pre-GCNIS development in AIS but factors related to malignant progression remain unclear. Although data in older patients remain scarce, malignant progression appears to be a rare event, although the natural history of the premalignant lesion remains unknown. Therefore, the practice of routine prophylactic gonadectomy in adults with AIS appears questionable and the patient's preference, after having been fully informed, should be decisive in this matter.Study Funding/competing Interest(s): This study was supported by research grants from the Research Foundation Flanders (FWO) (to M.C.), the Conselho Nacional de Desenvolvimento Científico e Tecnológico (CNPq G0D6713N) (to B.B.M. and M.C.) and the European Society for Pediatric Endocrinology (ESPE), granted by Novo Nordisk AB (to J.K.). There are no competing interests. [ABSTRACT FROM AUTHOR]

Published

2017

26. On the origin of germ cell neoplasia in situ: Dedifferentiation of human adult Sertoli cells in cross talk with seminoma cells in vitro

Author

Roswitha Weigel, Daniel Nettersheim, Martin Bergmann, Nelli Baal, Carmen Schröck, Sabine Kliesch, Rajkumar Savai, Poonam Sarode, Hubert Schorle, Valérie Schumacher, Monika Kressin, Cornelia Fink, and Jochen Wilhelm

Subjects

Male, 0301 basic medicine, Cancer Research, Embryonic Germ Cells, Microenvironment, Cell Communication, Biology, Keratin 18, Embryonal carcinoma, 03 medical and health sciences, 0302 clinical medicine, SOX2, Germ cell neoplasia in situ, Cell Line, Tumor, Coculture model, Biomarkers, Tumor, medicine, Humans, RC254-282, Neoplasm Staging, Original Research, Sertoli cell dedifferentiation, Sertoli Cells, Intratubular germ cell neoplasia, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Seminoma, Cell Dedifferentiation, Neoplasms, Germ Cell and Embryonal, medicine.disease, Sertoli cell, Cell Transformation, Neoplastic, 030104 developmental biology, medicine.anatomical_structure, Gene Expression Regulation, Cell culture, 030220 oncology & carcinogenesis, Cancer research, Disease Susceptibility, TCam-2 seminoma cell line, Carcinoma in Situ

Abstract

Germ cell neoplasia in situ (GCNIS) is the noninvasive precursor of testicular germ cell tumors type II, the most common cancer in young men, which originates from embryonic germ cells blocked in their maturation. GCNIS is associated with impaired Sertoli cells (SCs) that express fetal keratin 18 (KRT18) and the pluripotency factor SRY-Box transcription factor 2 (SOX2). According to the current theory concerning the origin of GCNIS, these SCs are prepubertal cells arrested in their maturation due to (epi)genetic anomalies and/or environmental antiandrogens. Thus, they are unable to support the development of germ cells, which leads to their maturational block and further progresses into GCNIS. Alternatively, these SCs are hypothesized to be adult cells dedifferentiating secondarily under the influence of GCNIS. To examine whether tumor cells can dedifferentiate SCs, we established a coculture model of adult human SCs (FS1) and a seminoma cell line similar to GCNIS (TCam-2). After 2 wk of coculture, FS1 cells showed progressive expression of KRT18 and SOX2, mimicking the in vivo changes. TCam-2 cells showed SOX2 expression and upregulation of further pluripotency- and reprogramming-associated genes, suggesting a seminoma to embryonal carcinoma transition. Thus, our FS1/TCam-2 coculture model is a valuable tool for investigating interactions between SCs and seminoma cells. Our immunohistochemical and ultrastructural studies of human testicular biopsies with varying degrees of GCNIS compared to biopsies from fetuses, patients with androgen insensitivity syndrome, and patients showing normal spermatogenesis further suggest that GCNIS-associated SCs represent adult cells undergoing progressive dedifferentiation.

Published

2021

27. Can germ cell neoplasia in situ be diagnosed by measuring serum levels of microRNA371a-3p?

Author

Radtke, A., Cremers, J.-F., Kliesch, S., Riek, S., Junker, K., Mohamed, S., Anheuser, P., Belge, G., and Dieckmann, K.-P.

Subjects

*GERM cell tumors, *MICRORNA, *BLOOD testing, *IN situ hybridization, *IMMUNOHISTOCHEMISTRY

Abstract

Purpose: Diagnosing germ cell neoplasia in situ (GCNis) can detect germ cell tumours (GCTs) at the pre-invasive stage. To date, testicular biopsy with the potential of surgical complications is the only way of safely diagnosing GCNis. Recently, microRNAs (miRs) 371-3, and miR 367 were shown to be valuable serum biomarkers of GCTs. We explored the usefulness of these candidate miRs as a marker for GCNis. Methods: 27 patients with GCNis and no concomitant GCT were enrolled. All patients underwent measuring serum levels of miR-371a-3p and miR-367-3p before treatment, 11 had repeat measurement after treatment, 2 also had testicular vein blood examinations. Serum levels were measured by quantitative PCR. In addition, four orchiectomy specimens of patients with GCT were examined immunohistochemically and by in situ hybridization (ISH) with a probe specific for miR-371a-3p to look for the presence of this miR in GCNis cells. Results: The median serum level of miR-371a-3p was significantly higher in patients with GCNis than in controls, miR-367 levels were not elevated. Overall, 14 patients (51.9%) had elevated serum levels of miR-371a-3p. The highest levels were found in patients with bilateral GCNis. Levels in testicular vein serum were elevated in both of the cases. After treatment, all elevated levels dropped to normal. In two orchiectomy specimens, miR-371a-3p was detected by ISH in GCNis cells. Conclusions: Measuring miR-371a-3p serum levels can replace control biopsies after treatment of GCNis. In addition, the test can guide clinical decision making regarding the need of testicular biopsy in cases suspicious of GCNis. [ABSTRACT FROM AUTHOR]

Published

2017

28. Update on the Pathophysiology and Risk Factors for the Development of Malignant Testicular Germ Cell Tumors in Complete Androgen Insensitivity Syndrome.

Author

Cools, Martine and Looijenga, Leendert

Subjects

*GERM cell tumors, *ANDROGEN-insensitivity syndrome, *CARCINOMA in situ, *SEMINOMA, *SINGLE nucleotide polymorphisms, *CANCER risk factors, *TESTICULAR cancer, *THERAPEUTICS

Abstract

Prophylactic gonadectomy in young adult women with complete androgen insensitivity syndrome (CAIS) to avoid development of an invasive testicular germ cell tumor (TGCT) is currently advised in most centers. However, women with CAIS increasingly question the need of this procedure. In order to provide optimal counseling and follow-up of these women, insight in the mechanisms underlying TGCT development in androgen insensitivity syndrome (AIS), data regarding the incidence of TGCT in AIS adults specifically, and an overview of existing and novel screening tools for in situ and invasive neoplastic lesions are crucial. The current knowledge regarding these topics is revised in this paper. [ABSTRACT FROM AUTHOR]

Published

2017

29. Contralateral biopsies in patients with testicular germ cell tumours: What is the rationale?

Author

Oldenburg, Jan and Dieckmann, Klaus-Peter

Subjects

*GERM cells, *TUMORS, *BIOPSY, *TESTICULAR cancer, *EXPERT evidence

Abstract

Introduction: In 1979, the Copenhagen group around Dr. Skakkebaek introduced contralateral biopsy in patients with testicular germ cell tumour (GCT) as a means of early diagnosing a contralateral testicular tumour (Berthelsen et al. in Br Med J 2(6186):363-364, 1). Although the rationale of contralateral biopsies is based on much of scientific evidence, no issue regarding the management of GCTs has been more controversial than the issue of contralateral biopsies (Heidenreich in BJU Int 104(9 Pt B):1346-1350, 2; Grigor and Rorth in Eur Urol 23(1):129-135, 3). A poll conducted during the GCT Consensus Meeting in Berlin 2011 revealed that 43 % of 60 leading experts would not recommend a contralateral biopsy and only 13.7 % would do the biopsy in all cases with GCT (Beyer et al. in Ann Oncol 24(4):878-888, 4). Likewise, the European Association of Urology and the European Society of Medical Oncology offer only weak recommendations with respect to contralateral biopsies in their guidelines of testicular cancer (Albers et al. in Eur Urol 68(6):1054-1068, 5; Oldenburg et al. in Ann Oncol 24(Suppl 6):vi125-vi132, 6). Conclusion: This review summarizes contemporary knowledge regarding contralateral biopsies to provide professionals caring for GCT patients with sufficient information to decide for or against the procedure in clinical practice. [ABSTRACT FROM AUTHOR]

Published

2017

30. The plasticity of germ cell cancers and its dependence on the cellular microenvironment.

Author

Nettersheim, Daniel and Schorle, Hubert

Subjects

GERM cells, MATERIAL plasticity, SEMINOMA, SOX2 protein, GERM cell tumors, CARCINOGENESIS, DISEASE progression, CANCER

Abstract

So far, the understanding of germ cell cancer (GCC) pathogenesis is based on a model, where seminomas and non-seminomas represent distinct entities although originating from a common precursor termed germ cell neoplasia in situ (GCNIS). Embryonal carcinomas (ECs), the stem cell population of the non-seminomas, is pluri- to totipotent and able to differentiate into cells of all three germ layers, giving rise to teratomas or tumours mimicking extraembryonic tissues (yolk sac tumours, choriocarcinomas). With regard to gene expression, (epi)genetics and histology, seminomas are highly similar to GCNIS and primordial germ cells, but limited in development. It remains elusive, whether this block in differentiation is controlled by cell intrinsic mechanisms or by signals from the surrounding microenvironment. Here, we reviewed the recent literature emphasizing the plasticity of GCCs, especially of seminomas. We propose that this plasticity is controlled by the microenvironment, allowing seminomas to transit into an EC or mixed non-seminoma and vice versa. We discuss several mechanisms and routes of reprogramming that might be responsible for this change in the cell fate. We finally integrate this plasticity into a new model of GCC pathogenesis, allowing for an alternative view on the dynamics of GCC development and progression. [ABSTRACT FROM AUTHOR]

Published

2017

31. Germ cell neoplasia in situ: The precursor cell for invasive germ cell tumors of the testis.

Author

Spiller, Cassy M. and Bowles, Josephine

Subjects

*GERM cell tumors, *TESTICULAR diseases, *IN situ remediation, *HUMAN embryology, *FETAL development, *GENETICS

Abstract

Germ cell neoplasia in situ is the non-invasive precursor cell of origin for type II testicular germ cell tumors. It has long been postulated that germ cell neoplasia in situ is derived from defective germ cell development during embryonic life, and although it is impossible to trace in vivo the progression from fetal germ cell to germ cell neoplasia in situ to tumor, there is a large volume of evidence supporting this theory. Current studies focus on understanding how germ cell neoplasia in situ forms, how these cells are activated at puberty and how they transform to invasive tumors of various subtypes. Such information is informing novel diagnostic and therapeutic options. [ABSTRACT FROM AUTHOR]

Published

2017

32. The World Health Organization 2016 classification of testicular germ cell tumours: a review and update from the International Society of Urological Pathology Testis Consultation Panel.

Author

Williamson, Sean R, Delahunt, Brett, Magi‐Galluzzi, Cristina, Algaba, Ferran, Egevad, Lars, Ulbright, Thomas M, Tickoo, Satish K, Srigley, John R, Epstein, Jonathan I, Berney, Daniel M, Amin, Mahul B, Compérat, Eva, Humphrey, Peter A, Idrees, Muhammad T, Lopez‐Beltran, Antonio, Montironi, Rodolfo, Oliva, Esther, Perry‐Keene, Joanna, Verrill, Clare, and Yilmaz, Asli

Subjects

*GERM cell tumors, *UROLOGY, *TESTICULAR diseases, *PATHOLOGY, *ENDODERMAL sinus tumors

Abstract

Since the last World Health Organization (WHO) classification scheme for tumours of the urinary tract and male genital organs, there have been a number of advances in the understanding, classification, immunohistochemistry and genetics of testicular germ cell tumours. The updated 2016 draft classification was discussed at an International Society of Urological Pathology Consultation on Testicular and Penile Cancer. This review addresses the main updates to germ cell tumour classification. Major changes include a pathogenetically derived classification using germ cell neoplasia in situ (GCNIS) as a new name for the precursor lesion, and the distinction of prepubertal tumours (non-GCNIS-derived) from postpubertal-type tumours (GCNIS-derived), acknowledging the existence of rare benign prepubertal-type teratomas in the postpubertal testis. Spermatocytic tumour is adopted as a replacement for spermatocytic seminoma, to avoid potential confusion with the unrelated usual seminoma. The spectrum of trophoblastic tumours arising in the setting of testicular germ cell tumour continues to expand, to include epithelioid and placental site trophoblastic tumours analogous to those of the gynaecological tract. Currently, reporting of anaplasia (seminoma or spermatocytic tumour) or immaturity (teratoma) is not required, as these do not have demonstrable prognostic importance. In contrast, overgrowth of a teratomatous component (somatic-type malignancy) and sarcomatous change in spermatocytic tumour indicate more aggressive behaviour, and should be reported. [ABSTRACT FROM AUTHOR]

Published

2017

33. The biology of germ cell tumors in disorders of sex development.

Author

Hersmus, Remko, Bever, Yolande, Wolffenbuttel, Katja P., Biermann, Katharina, Cools, Martine, and Looijenga, Leendert H.J.

Subjects

*GERM cell tumors, *SEX differentiation disorders, *EPIGENETICS, *FETAL development, *SINGLE nucleotide polymorphisms

Abstract

Development of a malignant germ cell tumor, i.e., germ cell cancer ( GCC) in individuals with disorders of sex development ( DSD) depends on a number of (epi-)genetic factors related to early gonadal- and germ cell development, possibly related to genetic susceptibility. Fetal development of germ cells is orchestrated by strict processes involving specification, migration and the development of a proper gonadal niche. In this review we will discuss the early (epi-)genetic events in normal and aberrant germ cell and gonadal development. Focus will be on the formation of the precursor lesions of GCC in individuals who have DSD. In our view, expression of the different embryonic markers in, and epigenetic profile of the precursor lesions reflects the developmental stage in which these cells are blocked in their maturation. Therefore, these are not a primary pathogenetic driving force. Progression later in life towards a full blown cancer likely depends on additional factors such as a changed endocrine environment in a susceptible individual. Genetic susceptibility is, as evidenced by the presence of specific risk genetic variants ( SNPs) in patients with a testicular GCC, related to genes involved in early germ cell and gonadal development. [ABSTRACT FROM AUTHOR]

Published

2017

34. Germ Cell Neoplasia in Situ Recognized Incidentally with Complaining of Discomfort in the Right Testis: A Case Report.

Author

Takahashi K, Mizushima K, Yamazaki M, Takazawa N, Isobe H, Asahina M, Hirai S, and Horie S

Abstract

A 27-year-old man experienced discomfort in his right testis in early September, 2021, and visited the hospital five days later. Physical examination did not detect any abnormalities in the scrotum. However, an ultrasound revealed a tumor in the central part of the right testis, and a Magnetic Resonance Imaging (MRI) showed a tumor 2.7cm in diameter with clear boundaries and a marginally smooth surface. The level of alpha-fetoprotein, human chorionic gonadotropin, human chorionic gonadotropin-β subunit, and lactate dehydrogenase were within normal limits. A Computed Tomography (CT) scan showed no abnormalities. We can't rule out the possibility of malignancy, right radical orchiectomy was performed with a diagnosis of right testicular tumor in mid-September 2021. The macroscopic lesion was 1.5×1.3 cm in size, and no viable tumorous cells were found pathologically. Atypical cells were observed in the seminiferous tubules from the spermatic cord, which were positively stained with immune-histochemical staining CD117 (c-kit), D2-40, and MIB-1 but negatively with alpha-fetoprotein, human chorionic gonadotropin, and human chorionic gonadotropin-β subunit. The pathological diagnosis was germ cell neoplasia in situ, and no continuity was observed between these cells and bleeding necrosis. The patient has been followed up for 1 year and 4 months after surgery, with no recurrence or metastasis observed., Competing Interests: The Author declares that there are no conflicts of interest., (2023 ©The Juntendo Medical Society.)

Published

2023

35. Sexual Function and Quality of Life in a National Cohort of Survivors of Bilateral Testicular Cancer

Author

Michael Kreiberg, Julie Wang Skøtt, Niels V. Holm, Jakob Lauritsen, Mads Agerbaek, Mikkel Bandak, Christoffer Johansen, and Gedske Daugaard

Subjects

Male, Pediatrics, medicine.medical_specialty, Time Factors, Urology, 030232 urology & nephrology, Sexual dysfunction, Anxiety, Bilateral orchiectomy, 03 medical and health sciences, 0302 clinical medicine, Cancer Survivors, Testicular Neoplasms, Testicular cancer, Quality of life, Germ cell neoplasia in situ, Interquartile range, medicine, Humans, Testosterone deficiency, Patient Reported Outcome Measures, Fatigue, Depression, business.industry, Late effects, Intratubular germ cell neoplasia, Odds ratio, Middle Aged, Neoplasms, Germ Cell and Embryonal, medicine.disease, Sexual Dysfunction, Physiological, Cross-Sectional Studies, 030220 oncology & carcinogenesis, Quality of Life, medicine.symptom, business, Sexual function

Abstract

Background: Sexual function and quality of life remain unexplored among long-term survivors of bilateral testicular cancer (TC). Objective: To investigate sexual function, fatigue, anxiety, and depression among long-term survivors of bilateral TC (unilateral TC with contralateral germ cell neoplasia in situ [TC + GCNIS] or bilateral TC [BTC]). Design, setting, and participants: This was a cross-sectional study of 2479 long-term TC survivors, of whom 126 were treated with contralateral radiotherapy for GCNIS, 93 were treated with bilateral orchiectomy for BTC, and 2260 had unilateral TC (reference group). Outcome measurements and statistical analysis: Outcomes were assessed using validated questionnaires at a median time since diagnosis of 17 yr (interquartile range 12–23). Results for survivors of TC + GCNIS and of BTC were compared with those for the reference group. Adjustment was made for age and treatment for disseminated disease. Results and limitations: The age-adjusted risk of anxiety was significantly higher among BTC survivors (odds ratio 1.7, 95% confidence interval [CI] 1.1–2.8; p = 0.002) than in the reference group. Apart from a higher risk of reduced motivation among survivors of TC + GCNIS (β = 0.067, 95% CI 0.0013–0.13; p = 0.046) there were no significant differences between the groups. Limitations include the low number of cases with symptoms of depression. Conclusions: Survivors of BTC had a higher risk of anxiety but did not experience impairment of other aspects of quality of life when compared to survivors of unilateral TC. These results are of importance for evidence-based information on late effects for bilateral TC patients. Patient summary: We evaluated quality of life and sexual function among long-term survivors of bilateral testicular cancer. Reassuringly, we did not find impaired quality of life apart from a higher risk of anxiety when comparing survivors of bilateral testicular cancer with survivors of unilateral testicular cancer. Long-term survivors of bilateral testicular cancer had a higher risk of anxiety but not of sexual dysfunction when compared to long-term survivors of unilateral testicular cancer.

Published

2020

36. Fibrillin-1 (FBN-1) a new marker of germ cell neoplasia in situ.

Author

Cierna, Z., Mego, M., Jurisica, I., Machalekova, K., Chovanec, M., Miskovska, V., Svetlovsk, D., Kalavska, K., Rejlekova, K., Kajo, K., Mardiak, J., Babal, P., and Svetlovska, D

Subjects

*GLYCOPROTEINS, *GERM cells, *GERMPLASM, *ANAL intraepithelial neoplasia, *FIBRILLIN, *GERM cell tumors, *TESTIS tumors, *CARCINOMA in situ, *IMMUNOHISTOCHEMISTRY, *TISSUE arrays, *DIAGNOSIS

Abstract

Background: Germ cell neoplasia in situ (GCNIS), is preinvasive stage of testicular germ cell tumours (TGCTs). Fibrillins, which are integral components of microfibrils are suggested to be involved in cancer pathogenesis and maintenance of embryonic stem cells pluripotency. The aim of this study was to examine fibrillin-1 (FBN-1) expression in TGCTs patients.Methods: Surgical specimens from 203 patients with TGCTs were included into the translational study. FBN-1 expression was evaluated in the tumour tissue, in GCNIS and in adjacent non-neoplastic testicular tissue in all available cases. Tissue samples were processed by the tissue microarray method. FBN-1 was detected by immunohistochemistry using goat polyclonal antibody and the expression was evaluated by the multiplicative quickscore (QS).Results: The highest FBN-1 positivity was detected in GCNIS (mean QS = 11.30), with overexpression of FBN-1 (QS >9) in the majority (77.1 %) of cases. Expression of FBN-1 in all subtypes of TGCTs was significantly lower in comparison to expression in GCNIS (all p <0.001). Seminoma had significantly higher expression compared to EC, ChC and TER (all p <0.05), but not to YST (p = 0.84). In non-neoplastic testicular tissue the FBN-1 positivity was very low (mean QS = 0.02). Sensitivity, specificity, positive and negative predictive value of FBN-1 expression for diagnosis of GCNIS were 97.1, 98.8, 98.6 and 97.7 %.Conclusions: FBN-1 is overexpressed in TGCTs and especially in GCNIS when compared to non-neoplastic testicular tissue in patients with germ cell tumors and could be involved in germ cell neoplasia in situ development. [ABSTRACT FROM AUTHOR]

Published

2016

37. Immunohistochemical Expression of Preferentially Expressed Antigen in Melanoma (PRAME) in the Uninvolved Background Testis, Germ Cell Neoplasia in Situ, and Germ Cell Tumors of the Testis

Author

Costantino Ricci, Tania Franceschini, Francesca Giunchi, Marco Grillini, Francesca Ambrosi, Francesco Massari, Veronica Mollica, Maurizio Colecchia, Michelangelo Fiorentino, Ricci, Costantino, Franceschini, Tania, Giunchi, Francesca, Grillini, Marco, Ambrosi, Francesca, Massari, Francesco, Mollica, Veronica, Colecchia, Maurizio, and Fiorentino, Michelangelo

Subjects

Male, Germ cell tumors of the testis, Reprogramming, General Medicine, Neoplasms, Germ Cell and Embryonal, Seminoma, Testicular Neoplasms, Antigens, Neoplasm, Germ cell neoplasia in situ, PRAME, Testis, Humans, Germ cell tumors of the testi, Melanoma, Retrospective Studies

Abstract

Objectives Preferentially expressed antigen in melanoma (PRAME) has a key role in regulating pluripotency of primordial germ cells and in the development of germ cell tumors of the testis (GCTT). However, its immunohistochemical expression in normal testes and its neoplastic counterpart remain largely unknown. Methods We retrospectively investigated the expression of PRAME in 26 cases of GCTT, 21 cases of germ cell neoplasia in situ (GCNIS), and 17 cases of uninvolved background testes. Results We found that PRAME was expressed more strongly by seminomatous rather than nonseminomatous GCTT (P = .000) and by pure seminoma rather than the seminoma component of seminomatous/nonseminomatous GCTT (P = .025). In addition, GCNIS and uninvolved background testes displayed high levels of PRAME expression. Conclusions PRAME is an additional marker for the differential diagnosis of GCTT and could play a key role in the transition from seminomatous to nonseminomatous GCTT.

Published

2021

38. Consensus guide on prophylactic gonadectomy in different sex development.

Author

Guerrero-Fernández J, González-Peramato P, Rodríguez Estévez A, Alcázar Villar MJ, Audí Parera L, Azcona San Julián MC, Carcavilla Urquí A, Castaño González LA, Martos Tello JM, Mora Palma C, Moreno Macián MF, Yeste Fernández D, and Nistal M

Subjects

Humans, Consensus, Castration, Sexual Development, Neoplasms, Germ Cell and Embryonal surgery

Abstract

The risk of suffering from gonadal germ cell tumors (GCT) is increased in some patients with different sexual development (DSD), mainly in those with Y chromosome material. This risk, however, varies considerably depending on a multitude of factors that make the decision for prophylactic gonadectomy extremely difficult. In order to make informed recommendations on the convenience of this procedure in cases where there is potential for malignancy, this consensus guide evaluates the latest clinical evidence, which is generally low, and updates the existing knowledge in this field., (Copyright © 2022 SEEN and SED. Published by Elsevier España, S.L.U. All rights reserved.)

Published

2022

39. Assessment of piRNA biogenesis and function in testicular germ cell tumors and their precursor germ cell neoplasia in situ

Author

Yulia Skvortsova, Tatyana L. Azhikina, Ildar Gainetdinov, Alexey Klimov, Alexey A. Tryakin, and Sofia A. Kondratieva

Subjects

0301 basic medicine, Male, Cancer Research, endocrine system, GCNIS, Testicular Germ Cell Tumor, Germ cell cancer, Piwi-interacting RNA, piRNA, Biology, lcsh:RC254-282, Germline, 03 medical and health sciences, Testicular Neoplasms, Germ cell neoplasia in situ, Neoplasms, Gene expression, Testis, Genetics, medicine, Biomarkers, Tumor, Humans, RNA, Small Interfering, Nonseminoma, Gene, PIWI, urogenital system, Intratubular germ cell neoplasia, High-Throughput Nucleotide Sequencing, Seminoma, Neoplasms, Germ Cell and Embryonal, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Cell biology, Neoplasm Proteins, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Germ Cells, Oncology, Argonaute Proteins, Testicular germ cell tumor, Biogenesis, Research Article

Abstract

Background Aberrant overexpression of PIWI/piRNA pathway proteins is shown for many types of tumors. Interestingly, these proteins are downregulated in testicular germ cell tumors (TGCTs) compared to normal testis tissues. Here, we used germline and TGCT markers to assess the piRNA biogenesis and function in TGCTs and their precursor germ cell neoplasia in situ (GCNIS). Methods We used small RNA deep sequencing, qRT-PCR, and mining public RNAseq/small RNA-seq datasets to examine PIWI/piRNA gene expression and piRNA biogenesis at four stages of TGCT development: (i) germ cells in healthy testis tissues, (ii) germ cells in testis tissues adjacent to TGCTs, (iii) GCNIS cells and (iv) TGCT cells. To this end, we studied three types of samples: (a) healthy testis, (b) testis tissues adjacent to two types of TGCTs (seminomas and nonseminomas) and containing both germ cells and GCNIS cells, as well as (c) matching TGCT samples. Results Based on our analyses of small RNA-seq data as well as the presence/absence of expression correlation between PIWI/piRNA pathway genes and germline or TGCT markers, we can suggest that piRNA biogenesis is intact in germ cells present in healthy adult testes, and adjacent to TGCTs. Conversely, GCNIS and TGCT cells were found to lack PIWI/piRNA pathway gene expression and germline-like piRNA biogenesis. However, using an in vitro cell line model, we revealed a possible role for a short PIWIL2/HILI isoform expressed in TGCTs in posttranscriptional regulation of the youngest members of LINE and SINE classes of transposable elements. Importantly, this regulation is also implemented without involvement of germline-like biogenesis of piRNAs. Conclusions Though further studies are warranted, these findings suggest that the conventional germline-like PIWI/piRNA pathway is lost in transition from germ cells to GCNIS cells. Electronic supplementary material The online version of this article (10.1186/s12885-017-3945-6) contains supplementary material, which is available to authorized users.

Published

2018

40. Can germ cell neoplasia in situ be diagnosed by measuring serum levels of microRNA371a-3p?

Author

Stephan Riek, Arlo Radtke, Sabine Kliesch, Klaus-Peter Dieckmann, Gazanfer Belge, Salah A. Mohamed, Petra Anheuser, J.-F. Cremers, and K. Junker

Subjects

0301 basic medicine, Adult, Male, Cancer Research, medicine.medical_specialty, Pathology, Adolescent, Testicular vein, Original Article – Clinical Oncology, In situ hybridization, Biology, 03 medical and health sciences, 0302 clinical medicine, Testicular Neoplasms, Germ cell neoplasia in situ, Quantitative polymerase chain reaction, Internal medicine, medicine, Biomarkers, Tumor, Humans, Neoplasm Invasiveness, Orchiectomy, Stage (cooking), Testicular biopsy, Neoplasm Staging, Hematology, Germ cell tumour, microRNA, Intratubular germ cell neoplasia, General Medicine, Middle Aged, Neoplasms, Germ Cell and Embryonal, medicine.disease, Prognosis, Survival Rate, MicroRNAs, 030104 developmental biology, medicine.anatomical_structure, Oncology, medicine.vein, 030220 oncology & carcinogenesis, Concomitant, Case-Control Studies, Germ cell, Carcinoma in Situ, Follow-Up Studies

Abstract

Purpose Diagnosing germ cell neoplasia in situ (GCNis) can detect germ cell tumours (GCTs) at the pre-invasive stage. To date, testicular biopsy with the potential of surgical complications is the only way of safely diagnosing GCNis. Recently, microRNAs (miRs) 371-3, and miR 367 were shown to be valuable serum biomarkers of GCTs. We explored the usefulness of these candidate miRs as a marker for GCNis. Methods 27 patients with GCNis and no concomitant GCT were enrolled. All patients underwent measuring serum levels of miR-371a-3p and miR-367-3p before treatment, 11 had repeat measurement after treatment, 2 also had testicular vein blood examinations. Serum levels were measured by quantitative PCR. In addition, four orchiectomy specimens of patients with GCT were examined immunohistochemically and by in situ hybridization (ISH) with a probe specific for miR-371a-3p to look for the presence of this miR in GCNis cells. Results The median serum level of miR-371a-3p was significantly higher in patients with GCNis than in controls, miR-367 levels were not elevated. Overall, 14 patients (51.9%) had elevated serum levels of miR-371a-3p. The highest levels were found in patients with bilateral GCNis. Levels in testicular vein serum were elevated in both of the cases. After treatment, all elevated levels dropped to normal. In two orchiectomy specimens, miR-371a-3p was detected by ISH in GCNis cells. Conclusions Measuring miR-371a-3p serum levels can replace control biopsies after treatment of GCNis. In addition, the test can guide clinical decision making regarding the need of testicular biopsy in cases suspicious of GCNis.

Published

2017

41. The plasticity of germ cell cancers and its dependence on the cellular microenvironment

Author

Daniel Nettersheim and Hubert Schorle

Subjects

Male, embryonal carcinoma, 0301 basic medicine, endocrine system diseases, cellular plasticity, SOX2, Reviews, Review, Germ layer, Cell fate determination, Biology, urologic and male genital diseases, Embryonal carcinoma, 03 medical and health sciences, 0302 clinical medicine, Carcinoma, Embryonal, Cell Line, Tumor, germ cell neoplasia in situ, medicine, Humans, Choriocarcinoma, germ cell cancer, SOXB1 Transcription Factors, seminoma, Intratubular germ cell neoplasia, Teratoma, Totipotent, carcinoma in situ, reprogramming, Cell Differentiation, Cell Biology, Seminoma, Cellular Reprogramming, medicine.disease, microenvironment, Cell biology, Gene Expression Regulation, Neoplastic, Cell Transformation, Neoplastic, 030104 developmental biology, Cellular Microenvironment, 030220 oncology & carcinogenesis, Immunology, Hepatocyte Nuclear Factor 3-beta, Molecular Medicine, Female, Reprogramming, Signal Transduction, germ cell tumour

Abstract

So far, the understanding of germ cell cancer (GCC) pathogenesis is based on a model, where seminomas and non-seminomas represent distinct entities although originating from a common precursor termed germ cell neoplasia in situ (GCNIS). Embryonal carcinomas (ECs), the stem cell population of the non-seminomas, is pluri- to totipotent and able to differentiate into cells of all three germ layers, giving rise to teratomas or tumours mimicking extraembryonic tissues (yolk sac tumours, choriocarcinomas). With regard to gene expression, (epi)genetics and histology, seminomas are highly similar to GCNIS and primordial germ cells, but limited in development. It remains elusive, whether this block in differentiation is controlled by cell intrinsic mechanisms or by signals from the surrounding microenvironment. Here, we reviewed the recent literature emphasizing the plasticity of GCCs, especially of seminomas. We propose that this plasticity is controlled by the microenvironment, allowing seminomas to transit into an EC or mixed non-seminoma and vice versa. We discuss several mechanisms and routes of reprogramming that might be responsible for this change in the cell fate. We finally integrate this plasticity into a new model of GCC pathogenesis, allowing for an alternative view on the dynamics of GCC development and progression.

Published

2017

42. A Rare Case of Embryonal Carcinoma in a Patient with Turner Syndrome without Y Chromosomal Material but Mutations in KIT, AKT1, and ZNF358 Demonstrated Using Exome Sequencing

Author

Gravholt, CH, Dollerup, OL, Duval, L, Mejlgaard, E, Stribolt, K, Vang, S, Laursen, BE, Knudsen, M, Thorsen, K, Hersmus, Remko, Looijenga, LHJ (Leendert), Stochholm, K, and Pathology

Subjects

MALIGNANCY, MARKERS, Germ cell neoplasia in situ, FEATURES, UPDATE, Gonadoblastoma, CLINICAL-PRACTICE GUIDELINES, Dysgerminoma, GERM-CELL TUMORS, 45,X, DIAGNOSIS, CANCER, FEMALE

Abstract

Gonadoblastoma and malignant transformations thereof can occur in females with Turner syndrome (TS) and Y chromosomal material. However, in females with TS and no Y chromosomal material, this is rarely seen. We report a female with an apparent 45,X karyotype (in blood and tumor) who was diagnosed with a metastatic embryonal carcinoma. Exome sequencing of blood and the tumor was done, and no Y chromosomal material was detected, while predicted deleterious mutations in KIT (likely driver), AKT1, and ZNF358 were identified in the tumor. The patient was treated with chemotherapy (first-line: cisplatin, etoposide, and bleomycin; second-line: paclitaxel and gemcitabine), and after that surgical debulking was performed. She is currently well and without signs of relapse. We conclude that embryonal carcinoma can apparently occur in 45,X TS without signs of Y chromosomal material.

Published

2018

43. The biology of germ cell tumors in disorders of sex development

Author

Hersmus, R. (Remko), Bever, Y. (Yolande) van, Wolffenbuttel, K.P. (Katja), Biermann, K. (Katharina), Cools, M.B.C.M. (Martine), Looijenga, L.H.J. (Leendert), Hersmus, R. (Remko), Bever, Y. (Yolande) van, Wolffenbuttel, K.P. (Katja), Biermann, K. (Katharina), Cools, M.B.C.M. (Martine), and Looijenga, L.H.J. (Leendert)

Abstract

Development of a malignant germ cell tumor, i.e., germ cell cancer (GCC) in individuals with disorders of sex development (DSD) depends on a number of (epi-)genetic factors related to early gonadal- and germ cell development, possibly related to genetic susceptibility. Fetal development of germ cells is orchestrated by strict processes involving specification, migration and the development of a proper gonadal niche. In this review we will discuss the early (epi-)genetic events in normal and aberrant germ cell and gonadal development. Focus will be on the formation of the precursor lesions of GCC in individuals who have DSD. In our view, expression of the different embryonic markers in, and epigenetic profile of the precursor lesions reflects the developmental stage in which these cells are blocked in their maturation. Therefore, these are not a primary pathogenetic driving force. Progression later in life towards a full blown cancer likely depends on additional factors such as a changed endocrine environment in a susceptible individual. Genetic susceptibility is, as evidenced by the presence of specific risk genetic variants (SNPs) in patients with a testicular GCC, related to genes involved in early germ cell and gonadal development.

Published

2017

44. Update on the Pathophysiology and Risk Factors for the Development of Malignant Testicular Germ Cell Tumors in Complete Androgen Insensitivity Syndrome

Author

Cools, M.B.C.M. (Martine), Looijenga, L.H.J. (Leendert), Cools, M.B.C.M. (Martine), and Looijenga, L.H.J. (Leendert)

Abstract

Prophylactic gonadectomy in young adult women with complete androgen insensitivity syndrome (CAIS) to avoid development of an invasive testicular germ cell tumor (TGCT) is currently advised in most centers. However, women with CAIS increasingly question the need of this procedure. In order to provide optimal counseling and follow-up of these women, insight in the mechanisms underlying TGCT development in androgen insensitivity syndrome (AIS), data regarding the incidence of TGCT in AIS adults specifically, and an overview of existing and novel screening tools for in situ and invasive neoplastic lesions are crucial. The current knowledge regarding these topics is revised in this paper.

Published

2017

45. Fibrillin-1 (FBN-1) a new marker of germ cell neoplasia in situ

Author

Viera Miskovska, Michal Mego, Katarina Machalekova, Pavel Babal, Igor Jurisica, Katarina Rejlekova, Karol Kajo, Zuzana Cierna, Daniela Svetlovska, Katarina Kalavska, Michal Chovanec, and Jozef Mardiak

Subjects

Male, 0301 basic medicine, endocrine system, Cancer Research, Pathology, medicine.medical_specialty, Fibrillin-1, Sensitivity and Specificity, 03 medical and health sciences, 0302 clinical medicine, Testicular Neoplasms, Testicular cancer, Germ cell neoplasia in situ, Biomarkers, Tumor, Genetics, medicine, Humans, Tissue microarray, business.industry, Carcinoma in situ, Intratubular germ cell neoplasia, Seminoma, Neoplasms, Germ Cell and Embryonal, medicine.disease, Immunohistochemistry, 030104 developmental biology, Oncology, Tissue Array Analysis, 030220 oncology & carcinogenesis, Germ cell tumors, business, Fibrillin, Carcinoma in Situ, Research Article

Abstract

Background Germ cell neoplasia in situ (GCNIS), is preinvasive stage of testicular germ cell tumours (TGCTs). Fibrillins, which are integral components of microfibrils are suggested to be involved in cancer pathogenesis and maintenance of embryonic stem cells pluripotency. The aim of this study was to examine fibrillin-1 (FBN-1) expression in TGCTs patients. Methods Surgical specimens from 203 patients with TGCTs were included into the translational study. FBN-1 expression was evaluated in the tumour tissue, in GCNIS and in adjacent non-neoplastic testicular tissue in all available cases. Tissue samples were processed by the tissue microarray method. FBN-1 was detected by immunohistochemistry using goat polyclonal antibody and the expression was evaluated by the multiplicative quickscore (QS). Results The highest FBN-1 positivity was detected in GCNIS (mean QS = 11.30), with overexpression of FBN-1 (QS >9) in the majority (77.1 %) of cases. Expression of FBN-1 in all subtypes of TGCTs was significantly lower in comparison to expression in GCNIS (all p

Published

2016

46. CDX2 immunostaining in primary and metastatic germ cell tumours of the testis

Author

Hakan Vuruşkan, Berna Aytaç Vuruşkan, Fatma Öz Atalay, Uludağ Üniversitesi/Tıp Fakültesi/Cerrahi Patoloji Anabilim Dalı., Uludağ Üniversitesi/Tıp Fakültesi/Üroloji Anabilim Dalı., Atalay, Fatma Öz, Vuruşkan, Berna Aytaç, Vuruşkan, Hakan, and AAH-9746-2021

Subjects

0301 basic medicine, Male, Pathology, Yolk sac tumor, Intestinal metaplasia, Testis tissue, Germ cell cancer, Expression, CDX2 protein, human, Testis cancer, Diagnosis, differential, Procedures, Biochemistry, CDX2 transcription factor, Metastasis, 0302 clinical medicine, Immunoreactivity, Seminiferous tubule, Yolk-sac, Neoplasms, Testis, Germ cell tumor, Medicine, Choriocarcinoma, CDX2, Testis teratoma, Staining, Transcription Factor Cdx2, Cadherin, Homeobox Genes, Teratoma, General Medicine, Tumor localization, Immunohistochemistry, Seminoma, Retrospective study, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Differentiation, embryonic structures, Archival tissue, Differential diagnosis, Cancer tissue, Germ cell, Human, Adult, Transcription factor Cdx2, medicine.medical_specialty, Testicular neoplasms, Research & experimental medicine, Histopathology, Neoplasms, germ cell and embryonal, Major clinical study, Adenocarcinoma, Carcinomas, Article, 03 medical and health sciences, Immunohistochemical survey, Primary tumor, Origin, Germ cell neoplasia in situ, Tissue section, Genetics, Humans, Tumor marker, Medicine, research & experimental, Human tissue, Germ cell tumour, Testis tumor, Carcinoma, embryonal, business.industry, Pharmacology & pharmacy, Biochemistry (medical), Research Reports, Staining and labeling, Cell Biology, Marker, medicine.disease, digestive system diseases, Retrospective studies, 030104 developmental biology, Metabolism, Embryonal carcinoma, Colon epithelium, Homeobox, Biomarkers, tumor, Cancer patient, Gene expression, business, Controlled study, Immunostaining, Yolk sac

Abstract

ObjectiveTo evaluate the immunohistochemical staining pattern of caudal type homeobox 2 (CDX2) protein in germ cell tumours (GCTs) of the testis.MethodsThis study reassessed archival tissue samples collected from patients diagnosed with primary and metastatic testicular GCTs for CDX2 immunoreactivity using standard immunohistochemical techniques. Positive nuclear immunostaining was evaluated with regard to both the staining intensity and the extent of the staining.ResultsTissue sections from primary and metastatic testicular GCTs ( n = 104), germ cell neoplasia in situ (GCNis) ( n = 5) and benign testicles ( n = 15) were analysed. The GCNis and benign testicular tissues showed no immunoreactivity for CDX2. Strong and diffuse staining of CDX2 was demonstrated only in the mature colonic epithelium of teratomas in both primary and metastatic GCTs. CDX2 positivity in other tumours (one pure yolk sac tumour, one yolk sac component of a mixed GCT and one pure seminoma) was infrequent, and was only weak and focal.ConclusionsCDX2 immunostaining should be interpreted based on both the staining intensity and the extent of staining so as not to cause misdiagnosis. Teratomas with colonic-type epithelium should be considered in the differential diagnosis if a metastatic tumour with an unknown primary shows prominent CDX2 immunostaining.

Published

2016

47. Development of germ cell neoplasia in situ in chinchilla rabbits

Author

Vigueras-Villaseñor, Rosa María, Montelongo Solís, Paola, Chávez-Saldaña, Margarita, Gutiérrez-Pérez, Oscar, Cortés Trujillo, Lucero, and Rojas-Castañeda, Julio César

Subjects

Germ cell neoplasia in situ, c-kit, 6 - Ciencias aplicadas::61 - Medicina::616 - Patología. Medicina clínica. Oncología [CDU], POU5F1, Animal model, Rabbit

Abstract

The present study was designed to describe the development of germ cell neoplasia in situ in Chinchilla rabbit by administration of estradiol. The study was performed in rabbits distributed into two groups: control and 17 β-estradiol. The determination of histological alterations and POU5F1 and c-kit proteins employed as biomarkers for the diagnosis of this neoplasia was carried out. Testicular descent and complete spermatogenesis were observed in the control group. The protein biomarkers were negative. However, in the rabbits treated with estradiol, the testes remained undescended with the gonocytes undifferentiated to spermatogonia. There were histological lesions owing to germ cell neoplasia in situ and positive to POU5F1 and c-kit proteins. These findings indicate that the chinchilla rabbit is an ideal model to study this neoplasia in which the histological characteristics and biomarkers of the disease could be clearly observed. Using this model we suggested that the persisting gonocytes could be responsible for the development of germ cell neoplasia in situ.

Published

2016

48. Sexual Function and Quality of Life in a National Cohort of Survivors of Bilateral Testicular Cancer.

Author

Bandak M, Lauritsen J, Johansen C, Kreiberg M, Skøtt JW, Agerbaek M, Holm NV, and Daugaard G

Subjects

Anxiety epidemiology, Cancer Survivors, Cross-Sectional Studies, Depression epidemiology, Fatigue epidemiology, Humans, Male, Middle Aged, Neoplasms, Germ Cell and Embryonal pathology, Patient Reported Outcome Measures, Testicular Neoplasms pathology, Time Factors, Neoplasms, Germ Cell and Embryonal therapy, Quality of Life, Sexual Dysfunction, Physiological epidemiology, Testicular Neoplasms therapy

Abstract

Background: Sexual function and quality of life remain unexplored among long-term survivors of bilateral testicular cancer (TC)., Objective: To investigate sexual function, fatigue, anxiety, and depression among long-term survivors of bilateral TC (unilateral TC with contralateral germ cell neoplasia in situ [TC+GCNIS] or bilateral TC [BTC])., Design, Setting, and Participants: This was a cross-sectional study of 2479 long-term TC survivors, of whom 126 were treated with contralateral radiotherapy for GCNIS, 93 were treated with bilateral orchiectomy for BTC, and 2260 had unilateral TC (reference group)., Outcome Measurements and Statistical Analysis: Outcomes were assessed using validated questionnaires at a median time since diagnosis of 17 yr (interquartile range 12-23). Results for survivors of TC+GCNIS and of BTC were compared with those for the reference group. Adjustment was made for age and treatment for disseminated disease., Results and Limitations: The age-adjusted risk of anxiety was significantly higher among BTC survivors (odds ratio 1.7, 95% confidence interval [CI] 1.1-2.8; p=0.002) than in the reference group. Apart from a higher risk of reduced motivation among survivors of TC+GCNIS (β=0.067, 95% CI 0.0013-0.13; p=0.046) there were no significant differences between the groups. Limitations include the low number of cases with symptoms of depression., Conclusions: Survivors of BTC had a higher risk of anxiety but did not experience impairment of other aspects of quality of life when compared to survivors of unilateral TC. These results are of importance for evidence-based information on late effects for bilateral TC patients., Patient Summary: We evaluated quality of life and sexual function among long-term survivors of bilateral testicular cancer. Reassuringly, we did not find impaired quality of life apart from a higher risk of anxiety when comparing survivors of bilateral testicular cancer with survivors of unilateral testicular cancer., (Copyright © 2018 European Association of Urology. Published by Elsevier B.V. All rights reserved.)

Published

2020

49. cd44 deletion suppresses atypia in the precancerous mouse testis.

Author

Li H, Shukla S, Frappart L, Herrlich P, and Ploubidou A

Subjects

Animals, Biomarkers, Tumor genetics, Carcinoma in Situ genetics, Carcinoma in Situ metabolism, Female, Infertility, Male genetics, Infertility, Male metabolism, Male, Mice, Mice, Transgenic, Neoplasms, Germ Cell and Embryonal genetics, Neoplasms, Germ Cell and Embryonal metabolism, Precancerous Conditions genetics, Precancerous Conditions metabolism, Sequence Deletion, Testicular Neoplasms genetics, Testicular Neoplasms metabolism, Carcinoma in Situ prevention & control, Extracellular Matrix Proteins physiology, Hyaluronan Receptors physiology, Infertility, Male prevention & control, Neoplasms, Germ Cell and Embryonal prevention & control, Precancerous Conditions prevention & control, Testicular Neoplasms prevention & control

Abstract

Loss-of-function of RHAMM causes hypofertility and testicular atrophy in young mice, followed by germ cell neoplasia in situ (GCNIS) of the testis, cellular atypia, and development of the testicular germ cell tumor (TGCT) seminoma. These pathologies reflect the risk factors and phenotypes that precede seminoma development in humans and-given the high prevalence of RHAMM downregulation in human seminoma-link RHAMM dysfunction with the aetiology of male hypofertility and GCNIS-related TGCTs. The initiating event underlying these pathologies, in RHAMM mutant testis, is premature displacement of undifferentiated progenitors from the basal compartment. We hypothesized that cd44 (both cancer initiating cell- and oncogenic progression marker) will drive GCNIS development, induced by RHAMM-loss-of-function in the mouse. We report that cd44 is expressed in a specific subset of GCNIS testes. Its genetic deletion has no effect on GCNIS onset, but it ameliorates oncogenic progression. We conclude that cd44 expression, combined with RHAMM dysfunction, promotes oncogenic progression in the testis., (© 2018 Wiley Periodicals, Inc.)

Published

2019

50. [Testicular germ cell tumors: Histopathological and molecular features].

Author

Tourne M, Radulescu C, and Allory Y

Subjects

Age Factors, Carcinoma, Embryonal classification, Carcinoma, Embryonal genetics, Carcinoma, Embryonal pathology, Choriocarcinoma classification, Choriocarcinoma genetics, Choriocarcinoma pathology, Choriocarcinoma, Non-gestational classification, Choriocarcinoma, Non-gestational genetics, Choriocarcinoma, Non-gestational pathology, Gene Deletion, Humans, Immunohistochemistry, Male, Mutation genetics, Neoplasms, Germ Cell and Embryonal classification, Seminoma classification, Seminoma genetics, Seminoma pathology, Teratoma classification, Teratoma genetics, Teratoma pathology, Terminology as Topic, Testicular Neoplasms classification, Neoplasms, Germ Cell and Embryonal genetics, Neoplasms, Germ Cell and Embryonal pathology, Testicular Neoplasms genetics, Testicular Neoplasms pathology

Abstract

In 2016, the WHO classification of testicular germ cell tumors was revised considering advances in the understanding of their tumorigenesis and molecular features. This restructuring led to a division into two major groups with, on one hand, prepubertal-type tumors, not derived from germ cell neoplasia in situ (GCNIS), and on the other hand, postpubertal-type tumors, GCNIS-derived, which occur in youg men (seminoma and non seminomatous germ cell tumors - embryonal carcinoma, yolk sac tumor, teratoma and choriocarcinoma essentially). The term germ cell neoplasia in situ is consensually accepted as a new terminology for the precursor lesion. In this new classification, the term "spermatocytic seminoma" is replaced by "spermatocytic tumor", reclassified among non-GCNIS-derived tumors. The purpose of this change of nomenclature is to reflect the usually non-aggressive behaviour of this tumor and to avoid any confusion with usual seminoma. The spectrum of trophoblastic tumors continues to expand with the description of new rare entities such as the cystic trophoblastic tumor, the placental site trophoblastic tumor and the epithelioid trophoblastic tumor. This review aims to provide a focus on testicular germ cell tumors highlighting the new immunohistochemical and molecular features responsible for the restructuring of classification. The TNM staging is presented according to the AJCC 8th edition 2017 update., (Copyright © 2019 Société Française du Cancer. Published by Elsevier Masson SAS. All rights reserved.)

Published

2019