Introduction
Malignant rhabdoid tumours (MRTs) of the kidney are
rare tumours that occur mainly in children (1). Cases of adult patients with renal MRT
are extremely rare, with <20 such cases reported in the
literature to date (2–5). The hSNF/INI1/SMARCB1/BAF47 gene is
hypothesized to act as a suppressor gene, and INI1 is expressed in
normal cells throughout the body (6). Loss and inactivation of INI1 expression
are associated with the development of MRT, atypical teratoid or
rhabdoid tumour of the central nervous system in children,
epithelioid sarcoma, collecting duct carcinoma, and epithelioid
malignant peripheral nerve sheath tumour (7–11). We
herein present a case of an adult patient with MRT of the left
kidney with associated loss of INI1 expression and multiple
metastatic lesions in the bones and lymph nodes.
Case report
A 79-year-old Japanese woman was admitted to Toyooka
Hospital (Toyooka, Japan) on the 1st December 2016, complaining of
pain in the right buttock and difficulty in ambulation. A computed
tomography (CT) scan revealed a thoracic and lumbar spine
deformity, narrowing of the spinal canal, and a tumour in the left
kidney. The patient's medical history included a cerebral
infarction at the age of 64 years, with no associated family
history. Laboratory tests were performed at the time of the
hospital visit and the results were as follows: C-reactive protein
and KL-6 increase to 12.0 mg/dl (normal, <0.3 mg/dl) and 558
U/ml (normal, <500 U/ml), respectively; the urinary cytology was
positive, suggesting malignancy.
An abdominal CT scan revealed a tumour sized 63×48
mm extending towards the upper pole of the left kidney (Fig. 1). Invasion of the tumour into the
renal pelvis was noted. The CT scan also revealed enlargement of
the renal hilar and para-aortic lymph nodes. Bone scintigraphy
demonstrated multiple bone metastatic lesions in the thoracic and
lumbar spine, the skull and the pelvic bones (Fig. 2). These bone metastases were
considered to be the cause of the pain in the buttock and
difficulty in ambulation.
Percutaneous needle biopsy of the renal tumour was
performed under echocardiographic guidance, followed by
histological examination. Three samples were obtained, all of which
contained atypical large tumour cells, with a small area of normal
renal tissue (Fig. 3A and B). The
tumour cells were large with round to polygonal shape, with
eccentrically positioned nuclei and prominent nucleoli. The
cytoplasm of the tumour cells was abundant and eosinophilic,
resembling the so-called ‘rhabdoid features’ (12). No other histological tumour types
were identified. Immunohistochemically, the tumour cells were
positive for vimentin, epithelial membrane antigen, CAM 5.2
(Fig. 3C-E) and p53, and negative
for cytokeratin (CK)7, CK20, α-methylacyl-CoA racemase, S100, CD45,
RCC-marker, anaplastic lymphoma kinase, α-smooth muscle actin,
desmin, MyoD1, myogenin, human melanoma black 45 and melan A (data
not shown). The tumour cells were also negative for INI1, although
lymphoid cells infiltrating among the tumour cells were positive
for INI1 (Fig. 3F). A small part of
the tumour was positive for CK(AE1/AE3) and CD10 (data not shown).
Based on the microscopic morphology and the immunohistochemical
examination, particularly the tumour cells staining negative for
INI1, the tumour was diagnosed as a renal MRT.
Based on the clinical data, the tumour was stage
cT1bN2M1 and had a score of 3 (poor risk group) in the Memorial
Sloan-Kettering Cancer Centre (MSKCC) Motzer Score for metastatic
RCC (13). Histological examination
also suggested a poor prognosis. A tyrosine kinase inhibitor,
axitinib, was administered. However, tumour growth continued,
resulting in an enlargement of the original renal tumour and the
metastatic lesions, and an increase in the number of metastatic
lesions (Fig. 4). KL-6 also
increased to 1,600 U/ml 3 months after treatment initiation. The
patient's general condition gradually worsened due to the growth of
the original tumour, the metastatic lesions, and the side effects
of the medication (including coughing and the elevation of
sialylated carbohydrate antigen KL-6), resulting in treatment
discontinuation (14). The patient
succumbed to the disease 3.5 months after the treatment
initiation.
Discussion
MRT development is associated with the loss of INI-1
expression (15–18). Biegel et al examined 18
patients with atypical teratoid rhabdoid tumours (ATRTs) of the
brain, 7 patients with renal MRTs, and 4 patients with extrarenal
rhabdoid tumours (17). All tumours
harboured INI1 gene abnormalities, such as homozygous deletions or
mutations of one or more exons. Germline mutations of the INI1 gene
were identified in 4 of the 29 patients (3 of 7 patients with renal
MRTs). Pinto et al reported that ~80% of paediatric patients
with multifocal synchronous or metachronous ATRTs and non-central
nervous system MRTs exhibited heterozygous germline INI1
abnormalities (18). In experiments
on mice, homozygous knockout of the INI1 gene resulted in embryonic
lethality in utero. Although heterozygous knockout mice with
the INI1 gene appear to be normal at birth, the mice develop
tumours histologically similar to MRT in later life (6). These results suggest that INI1 is a
tumour suppressor gene, and abnormalities of the INI1 gene are
closely associated with the development of MRTs.
Although renal MRTs mainly occur in children, a few
cases of adult MRTs have been reported. In addition, in the adult
cases of MRT, loss of INI1 expression has also been reported in
rare cases (4,5). In the present case, we observed loss of
INI1 expression in the tumour. It was also observed that the normal
cells in the kidney of the patient expressed INI-1. Therefore, loss
of INI1 was specific to the tumour cells. In the experiments on
mice, the somatic cells of the heterozygous INI1-knockout mice
expressed INI1, while the MRTs arising in mice exhibited loss of
INI1 expression. Heterozygous abnormality of the INI1 gene has been
reported in some children with MRTs (17). We were unable to undertake genomic
analysis of the tumour in our patient; therefore, we were unable to
determine whether the patient had a heterogenous abnormality in the
INI1 gene or a normal INI1 gene within the somatic cells in her
body. It has been reported that some adult MRT types coexist with
other types of RCCs. In these cases, MRT is hypothesized to develop
from RCC. However, to the best of our knowledge, only two adult
MRTs with a confirmed loss of INI1 expression have been reported to
date, and these were both pure MRTs. Our patient also displayed MRT
histology alone, although only biopsy samples were obtained. From
the experimental results in knockout mice, the INI1 gene appears to
be a tumour-suppressor gene and has homogenous abnormalities, and
deletion or mutation of the INI1 gene accelerates the development
of MRT, without other gene abnormalities; however, the development
of MRTs from other types of RCC requires multiple gene
abnormalities. Therefore, it is recommended to examine INI1
expression in MRTs combined with other RCC types. Further studies
should be conducted to elucidate the mechanism underlying the loss
of INI1 expression and the development of MRT in adults.
Previous studies have reported that MRTs in adults
are associated with a poor prognosis. Our patient succumbed to the
disease 6 months after the symptoms first appeared, despite
receiving treatment. Hence, medications that can suppress activated
gene(s) through the loss of INI1 expression may prove to be of
therapeutic value in adult MRT.
Acknowledgements
The authors would like to thank Ms H. Ogaki, Mr. K.
Nagaoka, Mr. T. Kuge, and Mr. H. Takenaka of Toyooka Hospital for
their expert technical assistance.
Funding
No funding was received.
Availability of data and materials
The datasets used and/or analysed during the
performance of this study are available from the corresponding
author upon reasonable request.
Authors' contributions
YO, YA, TShi, YN, YTaki, JW, MU, TSa and SI designed
the study. YO, TShi, YTanaka, JW, MU, TSa and YA analysed and
interpreted the patient data. YO and YA were major contributors to
writing the manuscript. YN, YTanaka, YA and SI performed the
histological examination of the tumour specimens and YN and YTanaka
confirmed the final histological diagnosis.
Ethics approval and consent to
participate
This study was approved by the Ethics Committee of
Toyooka Hospital (Toyooka, Japan; reference no. 165), and the
patient's family provided written informed consent.
Patient consent for publication
The patient's family approved the publication of the
case details and associated images.
Competing interests
The authors declare that they have no competing
interests.
References
|
1
|
Vujanić GM, Sandstedt B, Harms D,
Boccon-Gibod L and Delemarre JF: Rhabdoid tumour of the kidney: A
clinicopathological study of 22 patients from the International
Society of Paediatric Oncology (SIOP) nephroblastoma file.
Histopathology. 28:333–340. 1996. View Article : Google Scholar : PubMed/NCBI
|
|
2
|
Lowe W, Weiss RM, Todd MB and True LD:
Malignant rhabdoid tumor of the kidney in an adult. J Urol.
143:110–112. 1990. View Article : Google Scholar : PubMed/NCBI
|
|
3
|
Zhao G, Na R, Yang Y and Han R: Pure
malignant rhabdoid tumor of the left kidney in an adult: A case
report and review of the literature. Oncol Lett. 5:1481–1484. 2013.
View Article : Google Scholar : PubMed/NCBI
|
|
4
|
Podduturi V, Campa-Thompson MM, Zhou XJ
and Guileyardo JM: Malignant rhabdoid tumor of the kidney arising
in an adult patient. Proc (Bayl Univ Med Cent). 27:239–241. 2014.
View Article : Google Scholar : PubMed/NCBI
|
|
5
|
Rao Q, Xia QY, Shen Q, Shi SS, Tu P, Shi
QL and Zhou XJ: Coexistent loss of INI1 and BRG1 expression in a
rhabdoid renal cell carcinoma (RCC): Implications for a possible
role of SWI/SNF complex in the pathogenesis of RCC. Int J Clin Exp
Pathol. 7:1782–1787. 2014.PubMed/NCBI
|
|
6
|
Roberts CW, Galusha SA, McMenamin ME,
Fletcher CD and Orkin SH: Haploinsufficiency of Snf5 (integrase
interactor 1) predisposes to malignant rhabdoid tumors in mice.
Proc Natl Acad Sci USA. 97:13796–13800. 2000. View Article : Google Scholar : PubMed/NCBI
|
|
7
|
Roberts CW and Biegel JA: The role of
SMARCB1/INI1 in development of rhabdoid tumor. Cancer Biol Ther.
8:412–416. 2009. View Article : Google Scholar : PubMed/NCBI
|
|
8
|
Sigauke E, Rakheja D, Maddox DL, Hladik
CL, White CL, Timmons CF and Raisanen J: Absence of expression of
SMARCB1/INI1 in malignant rhabdoid tumors of the central nervous
system, kidneys and soft tissue: An immunohistochemical study with
implications for diagnosis. Mod Pathol. 19:717–725. 2006.
View Article : Google Scholar : PubMed/NCBI
|
|
9
|
Hornick JL, Dal Cin P and Fletcher CD:
Loss of INI1 expression is characteristic of both conventional and
proximal-type epithelioid sarcoma. Am J Surg Pathol. 33:542–550.
2009. View Article : Google Scholar : PubMed/NCBI
|
|
10
|
Elwood H, Chaux A, Schultz L, Illei PB,
Baydar DE, Billis A, Sharma R, Argani P, Epstein JI and Netto GJ:
Immunohistochemical analysis of SMARCB1/INI-1 expression in
collecting duct carcinoma. Urology. 78:474.e1–e5. 2011. View Article : Google Scholar
|
|
11
|
Jo VY and Fletcher CD: Epithelioid
malignant peripheral nerve sheath tumor: Clinicopathologic analysis
of 63 cases. Am J Surg Pathol. 39:673–682. 2015. View Article : Google Scholar : PubMed/NCBI
|
|
12
|
Schmidt D, Harms D and Zieger G: Malignant
rhabdoid tumor of the kidney. Histopathology, ultrastructure and
comments on differential diagnosis. Virchows Arch A Pathol Anat
Histopathol. 398:101–108. 1982. View Article : Google Scholar : PubMed/NCBI
|
|
13
|
Mekhail TM, Abou-Jawde RM, Boumerhi G,
Malhi S, Wood L, Elson P and Bukowski R: Validation and extension
of the Memorial Sloan-Kettering prognostic factors model for
survival in patients with previously untreated metastatic renal
cell carcinoma. J Clin Oncol. 23:832–841. 2005. View Article : Google Scholar : PubMed/NCBI
|
|
14
|
Gunnarsson O, Pfanzelter NR, Cohen RB and
Keefe SM: Evaluating the safety and efficacy of axitinib in the
treatment of advanced renal cell carcinoma. Cancer Manag Res.
7:65–73. 2015. View Article : Google Scholar : PubMed/NCBI
|
|
15
|
Versteege I, Sévenet N, Lange J,
Rousseau-Merck MF, Ambros P, Handgretinger R, Aurias A and Delattre
O: Truncating mutations of hSNF5/INI1 in aggressive paediatric
cancer. Nature. 394:203–206. 1998. View
Article : Google Scholar : PubMed/NCBI
|
|
16
|
Rousseau-Merck MF, Versteege I, Legrand I,
Couturier J, Mairal A, Delattre O and Aurias A: hSNF5/INI1
inactivation is mainly associated with homozygous deletions and
mitotic recombinations in rhabdoid tumors. Cancer Res.
59:3152–3156. 1999.PubMed/NCBI
|
|
17
|
Biegel JA, Zhou JY, Rorke LB, Stenstrom C,
Wainwright LM and Fogelgren B: Germ-line and acquired mutations of
INI1 in atypical teratoid and rhabdoid tumors. Cancer Res.
59:74–79. 1999.PubMed/NCBI
|
|
18
|
Pinto EM, Hamideh D, Bahrami A, Orr BA,
Lin T, Pounds S, Zambetti GP, Pappo AS, Gajjar A, Agnihotri S and
Broniscer A: Malignant rhabdoid tumors originating within and
outside the central nervous system are clinically and molecularly
heterogeneous. Acta Neuropathol. 136:315–326. 2018. View Article : Google Scholar : PubMed/NCBI
|
