Experimental Rodent Models of Brainstem Tumors

Wu, Qingze; Tyler, Betty; Sukay, Lindsey; Rhines, Laurence D.; DiMeco, Francesco; Clatterbuck, Richard E.; Guarnieri, Michael; Carson, Benjamin S.

doi:10.1354/vp.39-3-293

Cited by 22 publications

(9 citation statements)

References 29 publications

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“…The brainstem glioma model was modified from the one as previously described [27,40]. The animals were anesthetized with ketamine (40mg/Kg) in combination with xylazine (10mg/Kg) administered intraperitoneally.…”

Section: Methodsmentioning

confidence: 99%

Brainstem glioma progression in juvenile and adult rats

Liu

Kashyap

et al. 2008

JNS

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Objective Brainstem gliomas are common in children and have the worst prognosis of any brain tumor in children. On the other hand, brainstem gliomas are rare in adult, and clinical studies have suggested different biological behavior between young and adult. The present study was designed to develop an orthotropic C6 brainstem glioma model in young and adult rats, and to investigate the tumor biological behavior in the two age groups. Methods C6 glioma cells were stereotactically implanted into the pons of young or adult male rats. Neurological presentation and survival time were recorded. Tumor proliferation and apoptosis in brainstem gliomas of young and adult rats were determined by immunohistochemical staining of Ki-67 and TUNEL assay, respectively. Results Striking difference were found between young and adult brainstem glioma in the onset of neurological signs, duration of symptoms, survival time, tumor growth pattern, as well as tumor proliferation and apoptosis. Relatively focal tumors were observed in adult rats harboring brainstem glioma, while diffusive tumors were found in young rats. Furthermore, brainstem gliomas in adult rats were less proliferative and had more apoptosis than those in young rats. Conclusion The present study demonstrated that C6 brainstem glioma model in young and adult rats closely imitates human brainstem glioma in neurological findings and histopathology. Our findings suggest that the different growth pattern and invasiveness of brainstem glioma between children and adult could be due to the different host cellular environments between the two age groups, hence, warrant further investigation of the different host-response between childhood and adult brainstem glioma in human.

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Section: Methodsmentioning

confidence: 99%

Brainstem glioma progression in juvenile and adult rats

Liu

Kashyap

et al. 2008

JNS

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“…4). 56,57,65,123 Wu et al 122 demonstrated that carboplatin could be locally delivered to neoplastic cells in a rat brainstem tumor model with mini-osmotic pumps, which resulted in a prolongation of survival. Moreover, Lonser et al 71 documented the safety of locally infused Gd-bound albumin via stereotactically implanted cannulas into large areas of the primate midbrain and pons, followed by other reports showing the safety of CED of chemotherapeutic agents, such as gemcitabine and carboplatin, infused into the primate brainstem, although dose-dependent toxicity has been found with carboplatin.…”

Section: New Therapeutic Perspective Strategiesmentioning

confidence: 99%

Treatment of diffuse intrinsic brainstem gliomas: failed approaches and future strategies

Frazier¹,

Lee²,

Thomale

et al. 2009

PED

125

107

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Diffuse intrinsic pontine gliomas constitute ~ 60–75% of tumors found within the pediatric brainstem. These malignant lesions present with rapidly progressive symptoms such as cranial nerve, long tract, or cerebellar dysfunctions. Magnetic resonance imaging is usually sufficient to establish the diagnosis and obviates the need for surgical biopsy in most cases. The prognosis of the disease is dismal, and the median survival is < 12 months. Resection is not a viable option. Standard therapy involves radiotherapy, which produces transient neurological improvement with a progression-free survival benefit, but provides no improvement in overall survival. Clinical trials have been conducted to assess the efficacy of chemotherapeutic and biological agents in the treatment of diffuse pontine gliomas. In this review, the authors discuss recent studies in which systemic therapy was administered prior to, concomitantly with, or after radiotherapy. For future perspective, the discussion includes a rationale for stereotactic biopsies as well as possible therapeutic options of local chemotherapy in these lesions.

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“…We observed significant morbidity in rats infused at 5 l/h for 7 days (8) but recognize that morbidity in rodent studies depends on the volume and site of the infusion (37). Recent studies have shown that 4 l of solution can be infused into the rat brainstem at rates of 30 l/h (33).…”

Section: Discussionmentioning

confidence: 95%

A Surgical Technique for Safely Placing a Drug Delivery Catheter into the Pons of Primates: Preliminary Results of Carboplatin Infusion

Storm¹,

Clatterbuck²,

Liu³

et al. 2003

Neurosurgery

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The pons of monkeys is safely accessed with a catheter for drug delivery by using a posterior midline approach. Clinical observations, radiographic imaging, and laboratory tests of animals infused with saline for 3 months or 0.26 mg/ml of carboplatin for 1 month were unremarkable. Neurotoxicity was seen with dose levels of 2.6 mg/ml of drug for 1 month. This procedure offers opportunities for examining the toxicity of brainstem antitumor therapy in primates.

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Experimental Rodent Models of Brainstem Tumors

Cited by 22 publications

References 29 publications

Brainstem glioma progression in juvenile and adult rats

Brainstem glioma progression in juvenile and adult rats

Treatment of diffuse intrinsic brainstem gliomas: failed approaches and future strategies

A Surgical Technique for Safely Placing a Drug Delivery Catheter into the Pons of Primates: Preliminary Results of Carboplatin Infusion

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