Robert A. Wade scite author profile

35S- and 3H-labeled S-2-(3-methylaminopropylamino)ethylphosphorothioic acid (WR-3689) have been synthesized in our laboratory and used to study organ and cellular level distribution in C3H/Km mice bearing RIF-1 tumors. Tissue biodistributions obtained with 35S-WR-3689 showed that blood levels peak at 15 min postinjection and decline gradually over 60 min. At 30 min after drug injection the highest uptake is in kidney and submandibular salivary gland, with lowest levels in brain and moderate to low levels in the RIF-1 tumor, comparable to levels in skin and muscle. High resolution diffusible substance autoradiography with 3H-WR-3689 reveals a homogenous distribution of label over cells in liver and lung and nonuniform distribution of silver grains over the cytoplasm of cells in the kidney cortex, parotid and submandibular salivary glands, and small intestine. There are no indications of preferential nuclear location of label from protective drug in any tissue. Correlations of biodistribution and autoradiography data with measures of radioprotection in different tissues will be useful in interpreting mechanisms of radioprotection with this phosphorothioate.

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In Pursuit of Higher Purity: Use of ¹³C NMR and ¹³C-Enriched Substrates To Trace Impurity Generation and Removal in the Synthesis of Atorvastatin

Wade¹,

Zennie²,

Briggs³

et al. 1997

Org. Process Res. Dev.

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Robert A. Wade

EFFERVESCENT ATOMIZATION AT INJECTION PRESSURES IN THE MPa RANGE

Synthesis, Biodistribution, and Autoradiography of Radiolabeled S-2-(3-Methylaminopropylamino)ethylphosphorothioic Acid (WR-3689)

In Pursuit of Higher Purity: Use of ¹³C NMR and ¹³C-Enriched Substrates To Trace Impurity Generation and Removal in the Synthesis of Atorvastatin

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Robert A. Wade

EFFERVESCENT ATOMIZATION AT INJECTION PRESSURES IN THE MPa RANGE

Synthesis, Biodistribution, and Autoradiography of Radiolabeled S-2-(3-Methylaminopropylamino)ethylphosphorothioic Acid (WR-3689)

In Pursuit of Higher Purity: Use of 13C NMR and 13C-Enriched Substrates To Trace Impurity Generation and Removal in the Synthesis of Atorvastatin

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In Pursuit of Higher Purity: Use of ¹³C NMR and ¹³C-Enriched Substrates To Trace Impurity Generation and Removal in the Synthesis of Atorvastatin