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1 It is well tolerated but more myelosuppressive.
2 in CLL, pentostatin appears to be the least myelosuppressive.
3 logs active in CLL, pentostatin may be least myelosuppressive.
4 microtubule-binding drugs might alter their myelosuppressive action, we tested their effect in cell
5 were sensitive to in vivo treatment with the myelosuppressive agent 7,12 Dimethylbenz[a]anthracene (D
7 roperty of gallium nitrate is that it is not myelosuppressive and it lacks cross-resistance to other
8 xicity studies indicated that ABDNAZ was not myelosuppressive and no dose-limiting toxicity was appar
9 ion, children received alternating blocks of myelosuppressive and non-myelosuppressive chemotherapy e
13 prophylactic levofloxacin on cycle 1 only of myelosuppressive cancer chemotherapy and on subsequent c
15 ogenitor cell (HPCs) was not inhibited by 13 myelosuppressive chemokines that normally inhibit prolif
18 t for the treatment of tumors in addition to myelosuppressive chemotherapeutic drugs and/or those tha
19 id cancers and lymphomas receiving cyclical, myelosuppressive chemotherapy (causing grade 4 neutropen
20 del that mimics the clinical consequences of myelosuppressive chemotherapy complicated by Pseudomonas
21 ternating blocks of myelosuppressive and non-myelosuppressive chemotherapy every 14 days for an inten
22 atients 5 years to 18 years of age receiving myelosuppressive chemotherapy for nonmyeloid malignancie
24 lso be offered to those receiving moderately myelosuppressive chemotherapy for solid tumours and lymp
28 ematopoietic stem cell transplantation after myelosuppressive chemotherapy is used for the treatment
29 e, administration of Mpl-L immediately after myelosuppressive chemotherapy or preparatory regimens fo
30 duration of intravenous antibiotic use after myelosuppressive chemotherapy or to enhance dose intensi
31 cycle use of pegfilgrastim with a moderately myelosuppressive chemotherapy regimen markedly reduced f
32 Recommendations: For patients undergoing myelosuppressive chemotherapy who have a hemoglobin (Hb)
34 en the duration of febrile neutropenia after myelosuppressive chemotherapy, effectively mobilize hema
35 and expansion of HSCs and progenitors after myelosuppressive chemotherapy, inflammatory stress, and
42 O may play an important role in reducing the myelosuppressive complications of naturally occurring an
43 ribed a mixed chimerism protocol that avoids myelosuppressive conditioning and permits hematopoietic
44 CD34(+) selection and reinfused after either myelosuppressive conditioning with cyclophosphamide (200
47 nt roles in signaling for IFNgamma and other myelosuppressive cytokine receptors as a common mediator
48 d hematopoietic progenitors treated with the myelosuppressive cytokine tumor necrosis factor-alpha (T
49 evidence suggests that enhanced oxidant and myelosuppressive cytokine-mediated apoptosis of hematopo
58 lls confers multilineage protection from the myelosuppressive effects of BCNU and suggest a possible
62 tunately, the mechanisms responsible for the myelosuppressive effects of the cytokine are incompletel
64 indicate that myeloid cell A2ARs have direct myelosuppressive effects that indirectly contribute to t
66 However, in stark contrast to hydroxyurea's myelosuppressive effects, pomalidomide augmented erythro
72 Cs enhanced hematopoietic recovery following myelosuppressive injury and restored endogenous HSC func
74 em as well as in vivo EC infusions following myelosuppressive injury in mice to demonstrate that aged
77 s HSC function at steady state and following myelosuppressive insult, in which inhibition of EC NF-ka
78 rity and duration of thrombocytopenia due to myelosuppressive irradiation, chemotherapy, or both.
83 ta indicates that for patients on moderately myelosuppressive out-patient chemotherapy, the greatest
85 e, and 36 mg/m2 idarubicin [FAI]) and a more myelosuppressive, reduced-intensity regimen (100 to 150
87 c cell transplantation following a minimally myelosuppressive regimen, consisting of 100 cGy total bo
89 that retain some toxicity, and (2) minimally myelosuppressive regimens that rely on immunosuppression
90 s and require hospitalization, and minimally myelosuppressive regimens that rely on immunosuppression
91 ical development will likely target the most myelosuppressive regimens, including those used in hemat
95 tarting dose of clofarabine (15 mg/m(2)) was myelosuppressive, requiring several dose de-escalations
97 in gene therapy applications to decrease the myelosuppressive side effects of TS-directed anticancer
102 f Tpo to speed red blood cell recovery after myelosuppressive therapy in vivo and to enhance colony-f
104 recurrent disease and (B) pts with no prior myelosuppressive therapy or newly diagnosed tumors for w
111 as a means to protect against dose-limiting myelosuppressive toxicity ensuing from chemotherapy comb
112 ecessary for on-going studies evaluating non-myelosuppressive transplant regimens for the induction o
113 stimulation and display slower recovery from myelosuppressive treatment, suggesting that combinatoria
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