A Pilot Clinical and Pharmacokinetic Study of Intracarotid Cisplatin and Bleomycin

Feun, Lynn G.; Savaraj, Niramol; Lee, Ya Yen; Landy, Howard J.; Martinez-Prieto, J.; Charnsangavej, C.; Post, Judith D.; Lee, K. F.; Wallace, Sidney; Bowen, Brian C.; Kochan, Jeffrey P.; Yung, W. K. Alfred

doi:10.1089/sct.1991.7.29

Cited by 5 publications

(4 citation statements)

References 6 publications

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“…Previous reports of intraarterial chemotherapy have described a wide range of complications depending on the infusion protocol, agent used, and catheterrelated technique (10,12,14,15,21,31,32).…”

Section: Analysis Of Complicationsmentioning

confidence: 99%

Intraarterial Chemotherapy for Brain Tumors by Using a Spatial Dose Fractionation Algorithm and Pulsatile Delivery

Gobin¹,

Cloughesy²,

Chow³

et al. 2001

Radiology

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Section: Analysis Of Complicationsmentioning

confidence: 99%

Intraarterial Chemotherapy for Brain Tumors by Using a Spatial Dose Fractionation Algorithm and Pulsatile Delivery

Gobin¹,

Cloughesy²,

Chow³

et al. 2001

Radiology

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“…Several trials combining BCNU and IA CDDP have been reported with survival times ranging from 8 weeks to 48 months for responders [17][18][19][20][21]. CDDP intraarterially has also been associated with bleomycin [22], BCNU and VM-26 [23], and etoposide [24]. The response rate in these trials ranged from 28% to 82% with survival times from 33 to 160 weeks.…”

Section: Discussionmentioning

confidence: 99%

Intra-arterial cisplatin in malignant brain tumors: incidence and severity of otic toxicity

Assietti

Olson

1996

J Neuro-Oncol

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Intra-arterial (IA) cisplatin is used to treat gliomas with the goal of maximizing drug concentration in the brain while minimizing systemic toxicity. The present study is based on the author's experience with IA cisplatin administration in 12 patients. The primary goal of the study was to document the extent of otic toxicity in these individuals. Hearing was tested clinically and with audiograms, before each IA cisplatin injection. Eight women and four men with a mean age of 39 1/2 years (range 22-61) were treated. Diagnoses included 7 glioblastoma multiformes, 4 anaplastic astrocytomas, and 1 gliosarcoma. Diagnosis was obtained by stereotactic biopsy in four and craniotomy for resection and debulking in eight. The mean number of IA injections per patient was 4.58 (range 3-6). The cisplatin dose was 60 mg/m2 with the average dose of cisplatin per cycle being 116 mg (range 96-130 mg). Eleven patients had the agent administered via the internal carotid and one received it by way of a vertebral artery. Nine of the twelve patients (75%) demonstrated pure tone loss, as measured by audiography, of greater than 15 dB in the higher frequencies range (> or = 3 kHz) bilaterally. One patient became deaf and two others had clinically significant hearing loss. The severity of the auditory damage increased after each administration in each of the cases with clinical abnormality. IA cisplatin may have a role in the treatment of patients with primary malignant brain tumors, but further developments to limit otic toxicity would be of value.

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“…The CNS toxicity and lack of efficacy associated with the intra-carotid delivery of nitrosoureas in phase II studies (12) lead to the evaluation of less lipophilic though "active" agents or combinations of agents (carboplatin, cisplatin, bleomycin , etoposide, TNF-alpha) delivered by the intra-carotid route for the treatment of malignant glioma (13)(14)(15)(16)(17).…”

Section: Intra-carotid Delivery Of Chemotherapymentioning

confidence: 99%

Improving the delivery of therapeutic agents to CNS neoplasms: a clinical review

Badruddoja

Black²

2006

Front Biosci

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Even though nearly thirty-years of clinical research has attempted to improve the outcomes for patients with central nervous system neoplasms, the survival remains limited for a majority of these patients. Diverse intracellular signaling pathways involving apoptosis, invasion, angiogenesis and relevant mechanisms of resistance associated with CNS neoplasms are continuing to be elucidated. Phase I and II studies of systemically delivered chemotherapeutic agents and biological agents targeting these pathways have largely resulted in modest outcomes. Although the functional blood brain barrier was identified nearly eighty years ago only recently has the complexity and relevance of the blood brain-tumor barrier (BTB) been recognized as an important factor that limits the effective treatment of CNS neoplasms. Several groups have focused their efforts at improving the delivery of therapeutic agents across the blood brain-tumor barrier. The purpose of the article is to review novel methods that have attempted to improve the delivery of therapeutic agents into the CNS for the treatment of CNS neoplasm.

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A Pilot Clinical and Pharmacokinetic Study of Intracarotid Cisplatin and Bleomycin

Cited by 5 publications

References 6 publications

Intraarterial Chemotherapy for Brain Tumors by Using a Spatial Dose Fractionation Algorithm and Pulsatile Delivery

Intraarterial Chemotherapy for Brain Tumors by Using a Spatial Dose Fractionation Algorithm and Pulsatile Delivery

Intra-arterial cisplatin in malignant brain tumors: incidence and severity of otic toxicity

Improving the delivery of therapeutic agents to CNS neoplasms: a clinical review

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