Early and delayed neurotoxicity of Mitoxantrone and Doxorubicin following subarachnoid injection

Abstract: Doxorubicin (DXR) and Mitoxantrone (MXN) were administered into the subarachnoid space of mice or the ventricular system of rats. The maximal non-toxic systemic single dose (zero mortality = LDo) of DXR or MXN was used as reference for planning drug doses for CSF administration. LDo in mice were: 8 mg/kg DXR and 6 mg/kg MXN; in rats: 6 mg/kg DXR and 4.5 mg/kg MXN. Signs of neurotoxicity were remarkably similar in DXR or MXN treatment animals and included: head tremor, atactic-dystonic posture and circling beha… Show more

“…at P5. DOX is an antineoplastic agent that, when injected intraventricularly results in diffuse brain damage involving the forebrain and brainstem based on previous reports in adult rats(Siegal et al, 1988). Intracerebral injection of LPS in rat pups activates inflammatory cascades resulting in hypomyelination, white matter rarefaction and necrosis(Pang et al, 2003).…”

A model of symptomatic infantile spasms syndrome

“…at P5. DOX is an antineoplastic agent that, when injected intraventricularly results in diffuse brain damage involving the forebrain and brainstem based on previous reports in adult rats(Siegal et al, 1988). Intracerebral injection of LPS in rat pups activates inflammatory cascades resulting in hypomyelination, white matter rarefaction and necrosis(Pang et al, 2003).…”

A model of symptomatic infantile spasms syndrome

Pathophysiology of Catastrophic Epileptic Syndromes

Mechanisms of Neurotoxicity and Experimental Models