Human Germ Cell Tumors are Developmental Cancers: Impact of Epigenetics on Pathobiology and Clinic

Lobo, João; Gillis, Ad J. M.; Jerónimo, Carmen; Henrique, Rui; Looijenga, Leendert H. J.

doi:10.3390/ijms20020258

Cited by 98 publications

(83 citation statements)

References 160 publications

(174 reference statements)

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“…When refering to testicular cancer one is often referring, in fact, to testicular germ cell tumors (TGCTs), since they represent more than 95% of all testicular neoplasms. Despite not being a common malignancy, they are the most frequent solid cancers among young adult Caucasian men and incidence is increasing worldwide due to changes in lifestyle, which is in line with the proposed genetic and environmental model ("genvironment") of the disease [160][161][162].…”

Section: Major Clinical Challengessupporting

confidence: 63%

“…TGCTs are very heterogeneous [163], reflecting a complex tumor model that closely resembles developmental biology phenomena. Type II TGCTs (the most common) derive from a precursor lesion named germ cell neoplasia in situ (GCNIS), which then evolves into two big categories, seminomas (SEs) and non-seminomas (NSs), the latter being further divided into embryonal carcinoma (EC), postpubertal-type yolk sac tumor (YST), choriocarcinoma (CH) and postpubertal-type teratoma (TE) [162,164]. An integrated approach to TGCTs [165] has evidenced remarkable differences in methylation profiles between SE and NS, and also confirmed the value of the miR371-373 cluster in these tumors.…”

Section: Major Clinical Challengesmentioning

confidence: 99%

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Targeting the Immune system and Epigenetic Landscape of Urological Tumors

Lobo

Jerónimo

Henrique

2020

IJMS

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In the last years, we have witnessed remarkable advances in targeted therapies for cancer patients. There is a growing effort to either replace or reduce the dose of unspecific, systemic (chemo)therapies, given the associated short- and long-term side effects, by introducing more specific targeted therapies as single or combination agents. Due to the well-known implications of the immune system and epigenetic landscape in modulating cancer development, both have been explored as potential targets in several malignancies, including those affecting the genitourinary tract. As the immune system function is also epigenetically regulated, there is rationale for combining both strategies. However, this is still rather underexplored, namely in urological tumors. We aim to briefly review the use of immune therapies in prostate, kidney, bladder, and testicular cancer, and further describe studies providing supporting evidence on their combination with epigenetic-based therapies.

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Section: Major Clinical Challengessupporting

confidence: 63%

Section: Major Clinical Challengesmentioning

confidence: 99%

Targeting the Immune system and Epigenetic Landscape of Urological Tumors

Lobo

Jerónimo

Henrique

2020

IJMS

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“…Likewise, in an evaluation of miR-371a-3p expression levels in GCT subtypes by RNA extraction from formalin fixed paraffin embedded orchiectomy specimens, Vilela-Salgueiro et al revealed a strong expression in all GCT subtypes except teratoma [25]. The reason for the non-expression of the miR by teratoma is probably related to the analogies of GCT biology and the human embryonal development [34,35]. While most of the GCT subtypes mimic early developmental stages of embryonal development and accordingly retain their biochemical characteristics including the microRNA profile of stem cells, the teratoma subtype represents a more advanced and more mature histological subtype that has lost all of the biochemical characteristics of stem cells particularly the typical expression of miR-371a-3p [36].…”

Section: Intracellular Localization Of Mir-371a-3p By Ishmentioning

confidence: 99%

Graded expression of microRNA-371a-3p in tumor tissues, contralateral testes, and in serum of patients with testicular germ cell tumor

et al. 2020

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Copyright: Belge et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License 3.0 (CC BY 3.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. ABSTRACT Background: Serum levels of microRNA-371a-3p represent a specific tumor marker of testicular germ cell tumors (GCTs) but the origin of circulating miR-371a-3p is not finally resolved. The correlation between miR-levels in tissue and serum is unclear.Results: MiR-levels in GCT tissue are 399-fold higher than in contralateral testicular tissue and 5843-fold higher than in non-testicular tissue. MiR tissue levels correlate with corresponding serum levels (r 2 = 0.181). ISH detected miR-371a-3p intracellularly in GCT cells except teratoma. A low expression was also detected in normal testicular germ cells.Conclusions: Circulating miR-371a-3p is specifically derived from GCT tissue. The miR is present in GCT cells except teratoma. A low expression is also found in normal testicular tissue but not in non-testicular tissue. MiR-371a-3p levels in tissue and serum correlate significantly. This study underscores the usefulness of serum miR-371a-3p as tumor marker of GCT.Patients and methods: Expression levels of miR-371a-3p were concurrently measured in tissues of GCT, contralateral testes (n = 38), and in serum (n = 36) with real time PCR. For control, 5 healthy testicles and 4 non-testicular tissue samples were examined. MiR-levels were compared using descriptive statistical methods. We also performed in situ hybridization (ISH) of GCT tissue with a probe specific for miR-371a-3p.

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“…2 TGCTs are broadly divided into two main groups: those derived from the precursor lesion germ cell neoplasia in situ (GCNIS), generally called postpubertal-type tumors; and those unrelated to GCNIS. 3 The first group, on which we will be focusing, corresponds to type II TGCTs (within the developmental-based classification of these neoplasms 4,5 ), and include seminomas (SE) and non-seminomas (NS). NS can be further subdivided into embryonal carcinoma (EC), teratoma (TE), yolk-sac tumor (YST), and choriocarcinoma (CH), which are frequently admixed in the so-called mixed tumors.…”

Section: Introductionmentioning

confidence: 99%

p53 and MDM2 expression in primary and metastatic testicular germ cell tumors: Association with clinical outcome

et al. 2020

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Background Testicular germ cell tumors (TGCTs) are highly sensitive to platinum‐based chemotherapy, and wild‐type p53 seems to play a pivotal role in this susceptibility. On the other hand, overexpression of MDM2 seems to entail treatment resistance and unfavorable prognosis. Objectives We aimed to describe p53 and MDM2 immunoexpression in a well‐characterized cohort of primary and metastatic TGCTs and evaluate associations with clinicopathological and prognostic variables, including survival. Materials and methods 237 primary tumor samples and 12 metastases were evaluated for p53 and MDM2 immunoexpression using digital image analysis. Clinical records of all patients were reviewed for baseline clinical/pathologic characteristics and follow‐up. Results A significant positive correlation between p53 and MDM2 H‐scores was found (rs = 0.590, P < .0001). Non‐seminomas showed significantly higher expression levels of both p53 and MDM2 (P = .0002, P < .0001), which peaked in embryonal carcinomas and choriocarcinomas. Percentage of immunoexpressing cells and H‐score were significantly higher in chemo‐treated metastases compared with chemo‐naïve primary tumors for MDM2 (P ≤ .0001 for both), but not for p53 (P = .919 and P = .703, respectively). Cases with higher MDM2 immunoexpression showed a statistically significant trend for association with poorer prognosis (P = .043). Relapse/progression‐free survival at 12 months post‐diagnosis was lower in the “MDM2‐high” (≥P50) vs. the “MDM2‐low” (

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Human Germ Cell Tumors are Developmental Cancers: Impact of Epigenetics on Pathobiology and Clinic

Cited by 98 publications

References 160 publications

Targeting the Immune system and Epigenetic Landscape of Urological Tumors

Targeting the Immune system and Epigenetic Landscape of Urological Tumors

Graded expression of microRNA-371a-3p in tumor tissues, contralateral testes, and in serum of patients with testicular germ cell tumor

p53 and MDM2 expression in primary and metastatic testicular germ cell tumors: Association with clinical outcome

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