Cytogenetics of primary testicular nonseminoma, residual mature teratoma, and growing teratoma lesion in individual patients

Jannie Van Echten; Dirk T. Sleijfer; Janneke Wiersema; Heimen Schraffordt Koops; J. Wolter Oosterhuis; Bauke De Jong

doi:10.1016/S0165-4608(96)00284-1

Cytogenetics of primary testicular nonseminoma, residual mature teratoma, and growing teratoma lesion in individual patients

Jannie Van Echten
, Dirk T. Sleijfer
, Janneke Wiersema
, Heimen Schraffordt Koops
, J. Wolter Oosterhuis
, Bauke De Jong

Research output: Contribution to journal › Article › peer-review

22 Citations (Scopus)

Abstract

Residual mature teratoma (RMT) is often left behind when metastases of primary nonseminomatous germ cell tumors (NSs) are treated with chemotherapy. RMT is composed of fully differentiated somatic tissue. A growing teratoma (GTE) lesion may occur after (incomplete) resection of RMT. To shed light on tumor progression or the mechanism(s) of therapy related differentiation we investigated the chromosomal pattern of the primary NSs and RMTs in twelve patients, of the primary NS, RMT, and GTE lesion in one patient, and of the RMT and GTE lesion in two patients. Although several chromosomal differences are observed between the RMT and NSs and between the GTE and RMTs in the same patient, we obtained no evidence that specific chromosomal alteration(s) play a role in metastasis or differentiation.

Original language	English
Pages (from-to)	1-6
Number of pages	6
Journal	Cancer Genetics and Cytogenetics
Volume	96
Issue number	1
DOIs	https://doi.org/10.1016/S0165-4608(96)00284-1
Publication status	Published - 1 Jul 1997
Externally published	Yes

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title = "Cytogenetics of primary testicular nonseminoma, residual mature teratoma, and growing teratoma lesion in individual patients",

abstract = "Residual mature teratoma (RMT) is often left behind when metastases of primary nonseminomatous germ cell tumors (NSs) are treated with chemotherapy. RMT is composed of fully differentiated somatic tissue. A growing teratoma (GTE) lesion may occur after (incomplete) resection of RMT. To shed light on tumor progression or the mechanism(s) of therapy related differentiation we investigated the chromosomal pattern of the primary NSs and RMTs in twelve patients, of the primary NS, RMT, and GTE lesion in one patient, and of the RMT and GTE lesion in two patients. Although several chromosomal differences are observed between the RMT and NSs and between the GTE and RMTs in the same patient, we obtained no evidence that specific chromosomal alteration(s) play a role in metastasis or differentiation.",

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doi = "10.1016/S0165-4608(96)00284-1",

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T1 - Cytogenetics of primary testicular nonseminoma, residual mature teratoma, and growing teratoma lesion in individual patients

AU - Van Echten, Jannie

AU - Sleijfer, Dirk T.

AU - Wiersema, Janneke

AU - Koops, Heimen Schraffordt

AU - Oosterhuis, J. Wolter

AU - De Jong, Bauke

PY - 1997/7/1

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N2 - Residual mature teratoma (RMT) is often left behind when metastases of primary nonseminomatous germ cell tumors (NSs) are treated with chemotherapy. RMT is composed of fully differentiated somatic tissue. A growing teratoma (GTE) lesion may occur after (incomplete) resection of RMT. To shed light on tumor progression or the mechanism(s) of therapy related differentiation we investigated the chromosomal pattern of the primary NSs and RMTs in twelve patients, of the primary NS, RMT, and GTE lesion in one patient, and of the RMT and GTE lesion in two patients. Although several chromosomal differences are observed between the RMT and NSs and between the GTE and RMTs in the same patient, we obtained no evidence that specific chromosomal alteration(s) play a role in metastasis or differentiation.

AB - Residual mature teratoma (RMT) is often left behind when metastases of primary nonseminomatous germ cell tumors (NSs) are treated with chemotherapy. RMT is composed of fully differentiated somatic tissue. A growing teratoma (GTE) lesion may occur after (incomplete) resection of RMT. To shed light on tumor progression or the mechanism(s) of therapy related differentiation we investigated the chromosomal pattern of the primary NSs and RMTs in twelve patients, of the primary NS, RMT, and GTE lesion in one patient, and of the RMT and GTE lesion in two patients. Although several chromosomal differences are observed between the RMT and NSs and between the GTE and RMTs in the same patient, we obtained no evidence that specific chromosomal alteration(s) play a role in metastasis or differentiation.

UR - https://www.scopus.com/pages/publications/0031006287

U2 - 10.1016/S0165-4608(96)00284-1

DO - 10.1016/S0165-4608(96)00284-1

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AN - SCOPUS:0031006287

SN - 0165-4608

VL - 96

SP - 1

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JO - Cancer Genetics and Cytogenetics

JF - Cancer Genetics and Cytogenetics

IS - 1

ER -

Cytogenetics of primary testicular nonseminoma, residual mature teratoma, and growing teratoma lesion in individual patients

Abstract

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