Characteristics and Risk Factors of Cisplatin-Induced Ototoxicity in Testicular Cancer Patients Detected by Distorsion Product Otoacoustic Emission

Bíró, Krisztina; Noszek, László; Prekopp, Péter; Nagyiványi, Krisztián; Gergely, Lajos; Gaudi, István; Bodrogi, I.

doi:10.1159/000093776

Cited by 44 publications

(45 citation statements)

References 41 publications

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“…35 The increase in high frequencies pure tone thresholds was accompanied by significant decrease in the DPOAEs average SNR for 4000 to 8000 Hz in the control group confirming previous observations pointing to the organ of Corti outer hair cells as the primary target for Cisplatin ototoxicity. 31,32 The specific mechanisms involved in the attenuation of CIHL by Dexamethasone are not known yet. However, recent studies suggest the relevance of various cellular processes that might explain this otoprotection.…”

Section: Discussionmentioning

confidence: 99%

Prevention of Cisplatin‐Induced Hearing Loss by Intratympanic Dexamethasone: A Randomized Controlled Study

Marshak

Steiner

Kaminer

et al. 2014

Otolaryngol.--head neck surg.

110

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Section: Discussionmentioning

confidence: 99%

Prevention of Cisplatin‐Induced Hearing Loss by Intratympanic Dexamethasone: A Randomized Controlled Study

Marshak

Steiner

Kaminer

et al. 2014

Otolaryngol.--head neck surg.

110

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“…Audiologically, there are monitoring proposals using conventional frequencies (Testa et al 15 , Kushner et al 16 , Marshall et al 17 , Toral-Martinnon et al 18 ), monitoring proposals using transient otoacoustic emissions (Liberman 19 ) or distortion products (Biro et al 20 ; Hyppolito et al 21 ), and monitoring proposals using high frequencies (over 8000 Hz) (Garcia 22 ), which may be first affects by ototoxic drugs. In this case, patients with hearing loss normally do not complain and not always perceive loss of hearing (Liberman 23 ).…”

Section: Discussionmentioning

confidence: 99%

Report on hearing loss in oncology

Schultz¹,

Goffi-Gómez²,

Liberman³

et al. 2009

Braz. j. otorhinolaryngol. (Impr.)

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Ci splatin is used frequently as an antineoplastic drug in the treatment of many different cancers. However, when used in doses over 360mg/m 2 , ototoxicity may ensue, resulting in loss of hearing. Criteria for identifying and quantifying hearing loss have been devised. Aim: To describe the features of different hearing loss classification systems and to identify their implications and use in oncologic patients. Method: Hearing loss was classified in 31 patients before and after chemotherapy, according to different criteria, assessing the sensitivity and specificity of each classification system. Results: Hearing loss results were highly variable (ranging from 29% to 61%). Only 4 of 31 subjects with post-therapy hearing loss were identified by all the methods. A few subjects with hearing loss were classified as normal hearing in some of the criteria. A normal PTA was found in 18 of 31 subjects in the post-treatment evaluation. Conclusion: None of the criteria assesses the complaints of patients. The criteria described in this study were inadequate to identify hearing loss following chemotherapy, requiring additional information for physicians to better understand the hearing losses and their implications for the quality of life of patients.

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“…Indivíduos expostos a sons intensos ou a agentes ototóxicos podem apresentar mudanças na amplitude das EOA. Estudos relatam que, quando existem alterações de CCE, mesmo que ainda não exista mudança dos limiares tonais, já é possível observar uma redução da amplitude das EOA, demonstrando a sensibilidade deste parâmetro no diagnóstico precoce e/ou acompanhamento nos tratamentos quimioterápicos bem como nas questões de saúde do trabalhador [9][10][11][12] .…”

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Emissões otoacústicas produto de distorção em normo ouvintes e em perdas auditivas neurossensoriais leve e moderada com os protocolos 65/55 dB NPS E 70/70 dB NPS

et al. 2009

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RESUMOObjetivo: estudar comparativamente as amplitudes das emissões otoacústicas produto de distorção em indivíduos normo ouvintes, com perdas auditivas de graus leve e moderado. Métodos: a amostra compôs-se de 41 indivíduos na faixa etária de 18 a 45 anos, sendo 25 do sexo feminino e 16 do sexo masculino. Foram realizadas audiometrias tonal e vocal para classifi car os grupos conforme perfi l audiométrico; imitanciometria para avaliar as condições da orelha média; e emissões otoacústicas produto de distorção, utilizando os protocolos L1 = 65 dB NPS e L2 = 55 dB NPS e L1=L2= 70 dB NPS. No total, foram analisadas 63 orelhas (32 orelhas direitas e 31 orelhas esquerdas). Os indiví-duos selecionados foram distribuídos em três grupos distintos, sendo o primeiro grupo (G1) composto de 21 orelhas com audiometria tonal com limiares dentro da normalidade (grupo controle); o segundo grupo (G2) composto de 21 orelhas com perdas auditivas neurossensoriais de grau leve; e o terceiro grupo (G3) composto por 21 orelhas com perdas auditivas neurossensoriais de grau moderado. Os dados audiométricos foram comparados com os resultados das Emissões Otoacústicas Produto de Distorção (DPOAE). Resultados: encontrou-se diminuição e ausência das amplitudes no grupo com perda auditiva de grau leve (G2) e ausência de respostas no grupo com perda auditiva de grau moderado (G3) em ambos os protocolos. Conclusão: com relação ao grau da perda auditiva, pode-se concluir que quanto maior a perda auditiva, menor o aumento da amplitude das EOAPD.

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Characteristics and Risk Factors of Cisplatin-Induced Ototoxicity in Testicular Cancer Patients Detected by Distorsion Product Otoacoustic Emission

Cited by 44 publications

References 41 publications

Prevention of Cisplatin‐Induced Hearing Loss by Intratympanic Dexamethasone: A Randomized Controlled Study

Prevention of Cisplatin‐Induced Hearing Loss by Intratympanic Dexamethasone: A Randomized Controlled Study

Report on hearing loss in oncology

Emissões otoacústicas produto de distorção em normo ouvintes e em perdas auditivas neurossensoriais leve e moderada com os protocolos 65/55 dB NPS E 70/70 dB NPS

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