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Abstract
Purpose: To assess the therapeutic potential of methotrexate (MTX) and 5‐[125I]iodo‐2′‐deoxyuridine (125IdUrd) administered sequentially in rats bearing advanced (ten‐day‐old) intrathecal (i.t.) TE671 human rhabdomyosarcoma tumours.
Materials and methods: Nude rats were injected with TE671 cells through an i.t. placed catheter. Ten days later, the animals were injected i.t. over a 12‐day period with (i) saline daily, (ii) MTX every other day, (iii) 125IdUrd every other day, or (iv) MTX and 125IdUrd on alternating days. Onset of paralysis was determined as a function of time, and the medians for onset (M), percentage of cells killed (% kill), and log cell kill were calculated.
Results: The data show that (i) injection of MTX leads to a moderate delay in the onset of paralysis (MMTX=29 d versus Msaline=20 d), (ii) administration of 125IdUrd is more effective (MIdUrd=36 d), and (iii) sequential administration of MTX–125IdUrd further increases the therapeutic efficacy of 125IdUrd (MMTX–IdUrd=47 d).
Conclusions: Intrathecal injection of MTX–125IdUrd is efficacious in the therapy of advanced intrathecal tumours.