Martin I. Blake scite author profile

Cytopenia after high-dose chemotherapy and autologous stem cell reinfusion is a major cause of morbidity. Ex vivo cultured expansion and differentiation of CD34+ peripheral blood progenitor cells (PBPC) to neutrophil precursors may shorten the neutropenic period further. We explored the use of these ex vivo cultured PBPCs in nine patients with metastatic breast cancer. All underwent PBPC mobilization with cyclophosphamide, VP-16, and G-CSF. Subsequently, they underwent four to five apheresis procedures. One apheresis product from each patient was prepared using the Isolex 300 Magnetic Cell Separation System (Baxter Immunotherapy, Irvine, CA) to obtain CD34+ cells. These cells were then cultured in gas permeable bags containing serum-free X-VIVO 10 (BioWhittaker, Walkersville, MD) medium supplemented with 1% human serum albumin and 100 ng/mL PIXY321. At day 12 of culture the mean fold expansion was 26x with a range of 6 to 64x. One patient's cells did not expand because of a technical difficulty. The final cell product contained an average of 29.3% CD15+ neutrophil precursors with a range of 18.5% to 48.1%. The patients underwent high-dose chemotherapy with cyclophosphamide, carboplatin, and thiotepa. On day 0, the cryopreserved PBPCs were reinfused and on day +1 the 12-day cultured cells were washed, resuspended, and reinfused into eight of nine patients. One patient was not infused with cultured cells. The mean number of cultured cells reinfused was 44.6 x 10(6) cells/kg with a range of 0.8 to 156.6 x 10(6) cells/kg. No toxicity was observed after reinfusion. The eight patients have recovered absolute neutrophil counts > 500/microL on a median of 8 days (range 8 to 10 days); the median platelet transfusion independence occurred on day 10 (range 8 to 12 days) and platelet counts > 50,000/microL were achieved by day 12 (range 9 to 14) for the seven patients whose platelet counts could be determined. Expanded CD34+ selected PBPC can be obtained and safely reinfused into patients.

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Studies with Deuterated Drugs

Blake

Crespi

Katz

1975

Journal of Pharmaceutical Sciences

115

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Deuterium Isotope Effects in Transamination: L-Alanine and Pyridoxal

Blake¹,

Siegel²,

Katz³

et al. 1963

J. Am. Chem. Soc.

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The effect of placing electronegative substituents in the aliphatic portion of alkyl azides appears quite reasonable. By simple inductive means, they would tend to lower the energy of the electrons on NI, and thus increase the energies of both transitions. These are exactly the effects seen in the data of Tables I1 and 111. According to this, the effect should fall off rapidly with the distance of separation of the electronegative group and N1.

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Isolation of Fully Deuterated Metabolites from Scenedesmus obliquus Grown in Deuterium Oxide

Blake

Crespi

Mohan

et al. 1961

Journal of Pharmaceutical Sciences

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Determination of the pKa' Value for 5,5-Diphenylhydantoin

Agarwal

Blake

1968

Journal of Pharmaceutical Sciences

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Martin I. Blake

Selection and expansion of peripheral blood CD34+ cells in autologous stem cell transplantation for breast cancer

Studies with Deuterated Drugs

Deuterium Isotope Effects in Transamination: L-Alanine and Pyridoxal

Isolation of Fully Deuterated Metabolites from Scenedesmus obliquus Grown in Deuterium Oxide

Determination of the pKa' Value for 5,5-Diphenylhydantoin

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