C Berger scite author profile

Summary This study evaluates the degree and relevance of persisting ototoxicity after cisplatin-based standard-dose chemotherapy for testicular cancer, with emphasis on identification of potential factors for an increased risk of this late sequel. Hearing thresholds of 86 patients with a median age of 31 years (range 21-53 years) and a median follow-up time of 58 months (range 15-159 months) were assessed by conventional pure-tone audiometry. Interviews were conducted evaluating the patients' history with special regard to audiological risk factors, as well as circumstances of ototoxic symptoms. Details concerning treatment and patient variables were extracted retrospectively from the patients' charts. An additional screening programme assessed current body functions, blood parameters and other late toxicities. Symptomatic ototoxicity persisted in 20% of patients (59% tinnitus, 18% hearing loss, 23% both), while 10% had experienced completely reversible ototoxic symptoms for a duration of 1-18 months after treatment. Symptoms were bilateral in 81 % of patients. Hearing thresholds were compatible with cisplatin-induced hearing loss in 42% of audiograms performed. Subjective (history) and objective (audiogram) findings were not always consistent. The following statistically significant risk factors for ototoxicity were established: high cumulative dose of cisplatin (P < 0.0001); history of noise exposure (P = 0.006). Additionally, high doses of vincristine (P = 0.001) seemed to result in reversible ototoxic symptoms. No other independent risk factors were identified. In conclusion, persisting ototoxicity represents a clinical sequel for approximately 20% of testicular cancer patients treated at standard dose but may affect more than 50% of patients receiving cumulative doses of cisplatin > 400 mg m-2. Previous noise exposure may also result in a threefold increased risk for cisplatin ototoxicity. Future studies should use these risk factors as important stratification criteria for trials aiming at the evaluation and prevention of cisplatin-induced ototoxicity.Keywords: chemotherapy; ototoxicity; long-term toxicity; testicular cancerThe ototoxic potential of the chemotherapeutic agent cisplatin was recognized 2 decades ago (Piel et al, 1974). Despite the widespread use of cisplatin in standard treatment protocols for testicular, ovarian, head and neck, lung and other types of cancers, data on the frequencies of ototoxicity are not consistent, and risk factors have not been clearly identified so far. The measurement of the auditory function is limited because of the different diagnostic methods used for objective assessment and the subjective perception of symptoms; patients' characteristics, such as age or noise exposure, may additionally influence the hearing ability and different definitions of 'normal' and 'abnormal' hearing thresholds may also cause further discrepancies in reported results.In the current study the auditory function was evaluated in a homogeneous group of young men receiving cisplatin-based com...

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Evaluation of long-term toxicity after chemotherapy for testicular cancer.

Bokemeyer¹,

Berger²,

Kuczyk³

et al. 1996

JCO

248

122

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Secondary Raynaud's phenomenon and other late vascular complications following chemotherapy for testicular cancer

Berger

Bokemeyer

Schneider

et al. 1995

European Journal of Cancer

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Ifosfamide and etoposide in childhood osteosarcoma. A phase II study of the french society of paediatric oncology

Gentet¹,

Brunat‐Mentigny

Demaille

et al. 1997

European Journal of Cancer

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Endocrinological late effects after chemotherapy for testicular cancer

Berger

Bokemeyer²,

Schuppert³

et al. 1996

Br J Cancer

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Summary Type and extent of endocrinological alterations were studied in long-term disease-free survivors after cisplatin-based chemotherapy for testicular cancer. A total of 63 patients with a median age of 30 (19 -53) years, and median follow-up of 42 (16-128) months were included. Elevated serum follicle-stimulating hormone (FSH) levels were found in 63% of patients, 24% showed pathologically elevated luteinising hormone (LH) levels with normal and 10% with subnormal testosterone levels. The degree of gonadotropin elevation was highly significantly correlated with the cumulative platinum (P) dose. Patients treated with platinumvinblastine -bleomycin regimens showed higher gonadotropin levels than those treated with platinumetoposide-bleomycin. The adrenal androgen dehydroepiandrosterone (DHEA), pathologically elevated in 68% of patients, was significantly correlated with the cumulative doses of chemotherapy (ctx) used and to the gonadotropin levels. Treatment variables, such as type and dose of cytotoxic agents used, as well as degree of gonadotropin elevation were further correlated with changes in oestron, testosterone and 17a-OH-progesterone levels. Cholesterol levels were elevated in 32% of patients and significant interactions between the steroid hormone levels and cardiovascular risk factors could be shown.

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C Berger

Analysis of risk factors for cisplatin-induced ototoxicity in patients with testicular cancer

Evaluation of long-term toxicity after chemotherapy for testicular cancer.

Secondary Raynaud's phenomenon and other late vascular complications following chemotherapy for testicular cancer

Ifosfamide and etoposide in childhood osteosarcoma. A phase II study of the french society of paediatric oncology

Endocrinological late effects after chemotherapy for testicular cancer

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