Non-Wilms' Renal Tumors In Children:A 139 Cases Series

Background:Pediatric non-Wilms renal tumors (NWRTs) which comprise a small proportion of renal tumors,are a heterogeneous group of neoplasms with variable malignant potential, mortality, and response to treatment.This study aimed to determine the clinical characteristics, management and prognosis of children with non-Wilms' renal tumors(NWRTs). Methods:Medical records of all patients (n = 139) treated for NWRTs over a 12-year period (2008.01–2019.10) at a single center were reviewed retrospectively.Results:The histopathological groups of NWRTs included malignant rhabdoid tumor of the kidney(MRTK)(n: 30, 21.6%), renal cell cancer(RCC)(n: 26,18.7%), clear cell sarcoma of the kidney(CCSK)(n: 24,17.3%), congenital mesoblastic nephroma(CMN)(n: 21,15.1%), cystic nephroma(CN)(n: 16,11.5%),metanephric tumours(n: 12, 8.6%), renal angiomyoliporma(RAML)(n: 3, 2.2%), renal primitive neuroectodermal tumor(rPNET)(n: 2, 1.4%), renal hemangioma(n: 2, 1.4%), inflammatory myofibroblastic tumor(IMT)(n: 2, 1.4%), ossifying renal tumor of infancy(ORTI)(n: 1, 0.7%). 123 children were followed up with an average of 42 months. 16 children were lost to follow-up. Tumor-free survival was observed in 94 children. 28 children(22.8%) were died.Conclusions:Pediatric NWRTs comprises 19.1% of all renal tumors in our single center. Accurate diagnoses along with appropriate management are important factors in improving patients outcome. The mainstay treatment of malignant NWRTs including MRTK,CCSK,RCC and PNET is comprehensive treatment. The mainstay treatment of benign NWRTs including RAML,CN, ORTI, CMN,metanephric tumours, and renal hemangioma is surgical resection alone.

Pediatric cystic nephroma: clinical and molecular genetic characteristics

Cystic nephroma (CN) is a rare renal tumor occurring in children which belongs to a group of neoplasms linked with the inherited DICER1 syndrome. Given the rarity of CNs, it is important to describe clinical, radiological, and molecular genetic characteristics of these tumors in children and adolescents as well as to analyze treatment outcomes. We present our experience in managing 8 patients with histologically verified CN who received treatment and consultations at the D. Rogachev NMRCPHOI over a period of 9 years (2012–2020). The study was approved by the Independent Ethics Committee and the Scientific Council of the D. Rogachev NMRCPHOI. The patients’ parents gave their consent to the use of their child’s data, including photographs, for research purposes and in publications. We performed a retrospective analysis of clinical presentation, radiological findings, the extent of treatment given to patients, treatment outcomes, and the results of molecular genetic testing. The study included patients aged between 8.6 and 197 months at diagnosis (the median age was 14.2 months). The analysis of initial complaints revealed that six patients (75%) had an increased abdominal girth and a palpable mass in the abdomen, one patient (12.5%) presented with arterial hypertension, and another patient (12.5%) had a mass detected by a routine abdominal ultrasound examination. On contrast-enhanced computed tomography scans, CNs appeared as multicystic masses with thin, contrast-enhancing septa; the CN volume ranged from 59.7 to 1293.1 cm3 (the median volume was 626.3 cm3 ). In all cases, the diagnosis of CN was verified histologically. Surgical treatment included nephrectomy (n = 6) or partial resection of the affected kidney (n = 2) with the removal of the tumor. Some patients (n = 5) included in our analysis received pre-operative chemotherapy at the discretion of their treating physicians. Molecular genetic testing was carried out for 7 children: 4 out of 7 patients (57.1%) were found to have somatic and germline mutations in the DICER1 gene. Carriers of pathogenic DICER1 variant were identified in the family of 1 patient. The median duration of follow-up was 17.6 months (range: 1.7 to 58.9 months). Currently, all patients are alive, no relapses have occurred. Cystic renal neoplasms detected by radiological investigations should be reviewed at the reference centers for pediatric oncological diseases and included CN in the differential diagnosis. Initial surgery is the first line of treatment for cystic nephroma. The final diagnosis is made on the basis of a histological examination of tumor tissue. All patients with confirmed CN should be referred for genetic counseling and molecular genetic testing for germline mutations in the DICER1 gene and should receive surveillance recommendations for the early detection of other metachronous DICER1-associated tumors.

Cystic nephroma in pediatrics

El nefroma quístico es un tumor renal benigno raro, de etiología incierta. En niños puede manifestarse como una masa abdominal palpable, hematuria e infecciones urinarias recurrentes. Exámenes de imagen como ultrasonografía y tomografía computadorizada ayudan en el diagnóstico, sin embargo, la confirmación se realiza mediante el estudio anatomopatológico. El tratamiento es quirúrgico, pudiendo ser nefrectomía parcial o total, con buen diagnóstico.Objetivo: Describir un caso raro de nefroma quístico pediátrico, sus manifestaciones clínicas, aspectos radiológicos e histopatológicos, así como tratamiento y su evolución.Caso Clínico: Preescolar, sexo masculino, con historia clínica de infecciones urinarias de repetición en el primer año de vida. A los 2 años y 8 meses, presentó nodulación en hipocondrio derecho con dolor local a la palpación, asociado a molestias disúricas y hematuria. La ecografía mostró un riñón derecho aumentado de volumen por formación quística multiseptada. La tomografía computadorizada demostró formación expansiva quística multioculada en el riñón derecho. A los 2 años y 10 meses, realizó nefrectomía parcial derecha para exéresis y estudio anatomopatológico, compatible con nefroma quístico. Evolucionó con regresión de la hematuria y de los episodios recurrentes de infecciones urinarias, manteniendo función renal preservada. Actualmente, con 4 años y 6 meses, asintomático.Conclusiones: El nefroma quístico es una entidad rara, en general de buen pronóstico. La asociación de hallazgos clínicos, imágenes radiológicas y estudio anatomopatológico son fundamentales para el establecimiento diagnóstico y mejor definición de la conducta terapéutica.

Adult cystic nephroma masquerading urothelial carcinoma of a calyceal diverticulum

We report a complex cystic renal lesion in a 34-year-old man who presented with haematuria. It was managed by laparoscopic radical nephroureterectomy as it mimicked urothelial carcinoma.

Heterotopic Ossification in Benign and Malignant Renal Neoplasms

Introduction/Objective Heterotopic bone formation in renal neoplasms is a rare phenomenon. Ossification with or without marrow elements has been reported in both benign and malignant renal tumors. Due to its rarity, the epidemiological and clinical features of this finding are not well-documented. Herein, we have examined heterotopic ossification in renal neoplasms and summarized the epidemiological and clinical features of this entity. Methods/Case Report A database search on PubMed, Scopus, and Google Scholar was performed using a combination of proper search terms. Full article texts of all search results were reviewed with reference lists screened for additional articles matching the search criteria. The demographic details of the patients, disease characteristics, treatment, and outcomes were all extracted from full text articles and were summarized in a pre-standardized form. The inclusion criteria were set as any epithelial renal neoplasm with histological evidence of heterotopic ossification. A case of clear cell renal cell carcinoma (CCRCC) with heterotopic ossification diagnosed in our institution is included in the study. Results (if a Case Study enter NA) A total of 30 cases were found of renal neoplasms with bone formation. The majority of patients were between the ages of 40 to 60. The male to female ratio was 1:1. The majority (19/30) were histologically diagnosed as CCRCC, the most common subtype of kidney tumor with a few cases diagnosed as chromophobe RCC (4/30), papillary RCC (3/30), and cystic nephroma (2/30). Of the neoplasms reported, tumor size varied from 3.0 cm to 28.8 cm. Conclusion Heterotopic ossification of renal neoplasms often presents a diagnostic challenge to the radiologist as other benign conditions such as extramedullary hematopoiesis can be in the differential. The rarity of this phenomenon renders pre-surgical diagnosis difficult. Our study documents this phenomenon to be seen in a variety of renal neoplasms and underscores the necessity to be aware of this rare entity.

DICER1 tumor predisposition syndrome: an evolving story initiated with the pleuropulmonary blastoma

DICER1 syndrome (OMIM 606241, 601200) is a rare autosomal dominant familial tumor predisposition disorder with a heterozygous DICER1 germline mutation. The most common tumor seen clinically is the pleuropulmonary blastoma (PPB), a lung neoplasm of early childhood which is classified on its morphologic features into four types (IR, I, II and III) with tumor progression over time within the first 4–5 years of life from the prognostically favorable cystic type I to the unfavorable solid type III. Following the initial report of PPB, its association with other cystic neoplasms was demonstrated in family studies. The detection of the germline mutation in DICER1 provided the opportunity to identify and continue to recognize a number seemingly unrelated extrapulmonary neoplasms: Sertoli-Leydig cell tumor, gynandroblastoma, embryonal rhabdomyosarcomas of the cervix and other sites, multinodular goiter, differentiated and poorly differentiated thyroid carcinoma, cervical-thyroid teratoma, cystic nephroma-anaplastic sarcoma of kidney, nasal chondromesenchymal hamartoma, intestinal juvenile-like hamartomatous polyp, ciliary body medulloepithelioma, pituitary blastoma, pineoblastoma, primary central nervous system sarcoma, embryonal tumor with multilayered rosettes-like cerebellar tumor, PPB-like peritoneal sarcoma, DICER1-associated presacral malignant teratoid neoplasm and other non-neoplastic associations. Each of these neoplasms is characterized by a second somatic mutation in DICER1. In this review, we have summarized the salient clinicopathologic aspects of these tumors whose histopathologic features have several overlapping morphologic attributes particularly the primitive mesenchyme often with rhabdomyoblastic and chondroid differentiation and an uncommitted spindle cell pattern. Several of these tumors have an initial cystic stage from which there is progression to a high grade, complex patterned neoplasm. These pathologic findings in the appropriate clinical setting should serve to alert the pathologist to the possibility of a DICER1-associated neoplasm and initiate appropriate testing on the neoplasm and to alert the clinician about the concern for a DICER1 mutation.

Anaplastic Sarcoma of the Kidney With Heterologous Ganglioneuroblastic Differentiation: Another DICER1-Associated Tumor

Anaplastic sarcoma of the kidney (ASK) is a rare renal tumor for which less than thirty cases have been described in the literature to date. Diagnosis of ASK is primarily based on histology, which features solid spindle cell neoplastic islands arranged in a fascicular pattern, prominent anaplastic nuclear morphology, brisk mitoses, and multiple multiloculated cysts lined by hobnail epithelium reminiscent of cystic nephroma. Chondroid or rhabdomyocytic differentiation is often present within the sarcoma. It has been recently suggested that this tumor entity belongs to the DICER1 syndrome tumors based on identification of DICER1 mutations. We report on a case of this rare tumor found in a twenty-month-old female. In addition to the typical histologic findings of ASK, this case also displayed heterologous neuroblastic-gangliocytic differentiation, which has not been previously described in the literature. TP53 and BRAF v600E had aberrant immunostaining. Chromosomal microarray and genomic sequencing revealed loss of chromosome 10 p15.3-p11.2 and both somatic and germline DICER1 mutations, consistent with recent research and further supporting the classification of this tumor within the DICER1 syndrome associated tumors.

DICER1-Mutated Botryoid Fibroepithelial Polyp of the Parotid Duct: Report of the First Case

DICER1, a member of the ribonuclease III family, is involved in the biogenesis of microRNAs and, hence, it influences gene expression regulation. DICER1 germline (associated with the inherited DICER1 syndrome) or somatic mutations have been linked to tumorigenesis in histogenetically diverse benign and malignant neoplasms in different organs including pleuropulmonary blastoma, cystic nephroma, embryonal rhabdomyosarcoma, nasal chondromesenchymal hamartoma, poorly differentiated thyroid carcinoma, thyroblastoma, intracranial sarcoma and gonadal Sertoli-Leydig cell tumors in addition to others. Moreover, rare botryoid (giant) fibroepithelial polyps may harbor this mutation. Herein, we describe the first reported case of a DICER1-mutated botryoid fibroepithelial polyp occurring within the parotid duct of a 65-year-old female who has no other features or family history of the DICER1 syndrome. Based on its distinctive morphology, we tested this lesion specifically for DICER1 mutations and confirmed the presence of a pathogenic DICER1 variant with a low allele frequency, consistent with a somatic mutation.

Identification of a Novel DICER1 Germline Mutation in Thyroid Follicular Adenoma Using Whole Exome Sequencing

Backgrounds: DICER1 protein is a member of the ribonuclease III family of proteins that cleaves non-coding small RNA precursors to generate mature miRNAs, which in turn regulate gene expression post-transcriptionally. Thyroid abnormalities are frequently observed in DICER1 syndrome with multinodular goiter present in families in which a germline DICER1 mutation is segregating. Recently, we identified a germline DICER1 mutation in a family with multiple tumors using whole exome sequencing (WES). Methods and Materials: Following informed consent, WES of peripheral blood DNA was carried out on affected individual. Sanger sequencing was performed to confirm the DICER1 variant detected by WES and to assess her family for mutation in the same DICER1 exon (exon 20). Results: An 8 year-old girl presented with abdominal mass. Laparoscopic radical nephrectomy was done due to Wilms tumor. At age 12, palpable mass on the right thyroid lobe was found, and right hemithyroidectomy was performed. She was diagnosed with follicular adenoma, and she started to take levothyroxine. At age 13, palpable thyroid mass on the left thyroid lobe was identified, and total thyroidectomy was performed due to progressively enlarged remnant thyroid gland with multiple nodules. The pathological result was adenomatous goiter with a cystic change. During the evaluation, a 1.5cm follicular cyst in the left ovary, 0.7cm cystic lesion in the right middle lobe of the lung, and air-trappings in both lungs were observed. We performed WES which revealed a novel heterozygous missense mutation, c.3506C>G(p.S1169*) in exon 20 of the DICER1 gene. During the follow-up, she showed a severely enlarged right kidney with multiple septated cysts. Right total nephrectomy was done due to hemorrhage progression in cysts and biopsy revealed cystic nephroma. Continuous renal replacement therapy was applied after right nephrectomy, and maintenance hemodialysis was applied. Conclusions: We identified a novel DICER1 germline mutation in a family with thyroid follicular adenoma, Wilms tumor, and contralateral progressive cystic nephroma which is the first report in Korea.

Primary Biphasic Hepatic Sarcoma in DICER1 Syndrome

DICER1 tumor predisposition syndrome is a rare genetic disorder that predisposes individuals to multiple benign and malignant neoplasms. The phenotype is vast and includes pleuropulmonary blastoma (PPB), thyroid nodules, cystic nephroma, Wilms tumor, ovarian Sertoli–Leydig cell tumor, and medulloepithelioma, among others. Herein, we describe a patient with a DICER1 germline pathogenic variant presenting with two neoplasms that are not commonly encountered in the context of DICER1 syndrome. The first tumor is a multiloculated cystic hepatic lesion with a biphasic pattern, composed of cysts lined by bland biliary type (CK19-positive) epithelium surrounded by a condensation of sarcomatous spindled cell proliferation in a myxoid stroma. This neoplasm resembled PPB or cystic nephroma with malignant transformation. The second tumor is a chest nodule consistent with low-grade hidradenocarcinoma. Although it is difficult to speculate with just a single case, these unusual neoplasms occurring in particular at a young age raises the possibility that they can be inherent to, and thus, be part of the DICER1 tumor predisposition syndrome phenotype.