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1 gBRCA mutations or HRD status, with moderate bone marrow toxicity.
2 r frequencies and resistance to 5-FU-induced bone marrow toxicity.
3 ses beyond those levels which produce severe bone marrow toxicity.
4 locyte colony-stimulating factor to minimize bone marrow toxicity.
5 Ci/m2 of 125I-mAb A33 did not cause bowel or bone marrow toxicity.
6 = 0.009), generally for gastrointestinal or bone marrow toxicity.
7 ality associated with neutropenia and marked bone marrow toxicity.
8 ns to other participants, but none developed bone-marrow toxicity.
10 appears generally limited to mild transient bone marrow toxicity and xerostomia because of uptake of
12 ty profile, including no genotoxicity and no bone marrow toxicity at the highest evaluated concentrat
14 ations for the use of mouse models to assess bone marrow toxicity for DNA-damaging agents and inhibit
15 ceiving combined MMF and tacrolimus therapy; bone marrow toxicity in 24% of recipients receiving MMF
19 late-onset CMV disease, viral resistance and bone marrow toxicity limited enthusiasm for longer durat
23 prior to chemotherapy, the magnitude of the bone marrow toxicity nadir was minimized, even with BSO-
25 used with (131)I-tositumomab results in less bone marrow toxicity than does the weight-based dosing r
26 y, but their usefulness is limited by severe bone marrow toxicity that causes the cumulative depletio
27 represents a promising approach to overcome bone marrow toxicity, the limiting factor for most high-
29 esoporphyrin did not display any significant bone marrow toxicity when used at similar concentrations
30 de phosphate (2-fold) accompanied by greater bone marrow toxicity, whereas the acute toxicity of sodi
31 major limiting factor with this modality is bone marrow toxicity, which arises from the penetrating
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