Κ.S. Vitols scite author profile

Κ.S. Vitols

5Publications

113Citation Statements Received

88Citation Statements Given

How they've been cited

213

110

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Affiliations

Scripps Clinic, Scripps Health, Scripps Research Institute

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Studies on ferrochelatase. The effects of thiols and other factors on the determination of activity

Porra¹,

Vitols²,

Labbé³

et al. 1967

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1. Haems are unstable under aerobic conditions in the presence of thiols, which are used to activate the ferrochelatase enzyme; catalase inhibits this degradation of haem. In addition, thiols interfere with the determination of protohaem as its pyridine haemochromogen derivative. 2. Three ferrochelatase assays are described that minimize interference by these two reactions. Two of these assays involve measurement of porphyrin utilization, one spectrophotometrically and the second spectrofluorimetrically. The third assay measures haem formation by a pyridine haemochromogen technique. Results obtained with these three methods were in close agreement at a GSH concentration of 4mm. 3. The stimulatory effect of GSH on ferrochelatase has been confirmed. The spectrum of the haem formed is dependent on GSH concentration; at high GSH concentrations (20mm) the haem is in the reduced state, but at low concentration (4mm) the spectrum of the product resembles that of an oxidized haemoprotein such as ferrihaemoglobin. 4. The inhibitory effect of oxygen on ferrochelatase activity has been confirmed by spectrophotometric assay of porphyrin disappearance.

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Carboxypeptidase-mediated release of methotrexate from methotrexate .alpha.-peptides

Kuefner

Lohrmann²,

Montejano³

et al. 1989

Biochemistry

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Methotrexate (MTX) alpha-peptides containing representative neutral (alanine), acidic (aspartic acid), and basic (arginine) amino acids were synthesized by a regiospecific route. Purity and authenticity of MTX-Ala, MTX-Asp, and MTX-Arg were established by TLC, HPLC, elemental analysis, and NMR and absorbance spectra. These peptides were hydrolyzed by carboxypeptidases to yield MTX and the amino acids. Reactions were monitored by using a ninhydrin assay for the amino acids and HPLC and spectrophotometric assays for MTX. Pancreatic carboxypeptidase A (CP-A) hydrolyzed MTX-Ala and, at a much slower rate, MTX-Asp and MTX-Arg. MTX-Ala was also a substrate for pancreatic carboxypeptidase B (CP-B); marginal activity was observed with this enzyme and MTX-Arg. Human serum hydrolyzed only MTX-Arg; biphasic inhibition of this activity by 2-(mercaptomethyl)-3-(guanidinoethyl)thiopropionate was consistent with the known presence of two types of endogenous carboxypeptidase (CP-N). Cytotoxicity of the MTX peptides toward L1210 cells in culture was enhanced considerably in the presence of the appropriate carboxypeptidases. MTX-Ala was much less toxic than MTX (ID50 values of 2.0 X 10(-6) M and 2.4 x 10(-8) M, respectively), but in the presence of CP-A the ID50 of the peptide improved to 8.5 X 10(-8) M. Similar results were obtained with MTX-Asp/CP-A and MTX-Ala/CP-B combinations. MTX-Arg showed good cytotoxicity (ID50 of 5.0 X 10(-8) M), due to CP-N activity in the fetal bovine serum of the culture medium; inclusion of CP-B lowered the ID50 to that of MTX. Possible clinical uses of MTX peptides are discussed.

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The Reduction of Folate by Borohydride^*

Scrimgeour¹,

Vitols²

1966

Biochemistry

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Affinity labeling of folate transport proteins with the N-hydroxysuccinimide ester of .gamma.-isomer of fluorescein-methotrexate

Fan

Pope²,

Vitols³

et al. 1991

Biochemistry

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Fluorescein-methotrexate, a derivative in which the fluorophore is linked via a diaminopentane spacer to either the alpha- or gamma-carboxyl group of the glutamate moiety in the drug [Gapski et al. (1975) J. Med. Chem. 18, 526-528], has been synthesized by an improved procedure and separated by DEAE-Trisacryl chromatography into the alpha- and gamma-isomers (alpha-F-MTX and gamma-F-MTX). Each isomer was characterized by mass spectrometry, elemental analysis, absorbance spectrum, TLC, and reversed-phase HPLC. Identity of the isomers was established by the following enzymatic criteria: (a) gamma-F-MTX (but not the alpha-isomer) was hydrolyzed at the pteroate-glutamate bond by carboxypeptidase G2 to yield 4-amino-4-deoxy-10-methylpteroate and gamma-glutamyldiaminopentane-fluorescein; and (b) gamma-F-MTX was a much better inhibitor of human dihydrofolate reductase than the alpha-isomer (Ki values of 0.079 and 4.6 nM). alpha- and gamma-F-MTX were comparable as inhibitors (Ki values of 1.6 and 0.6 microM) of the transport system for reduced folates and MTX in L1210 cells, but the transporter in Lactobacillus casei was inhibited only by the gamma-isomer (Ki = 4.3 microM). The gamma-isomer, therefore, was selected for covalent labeling of proteins. When L. casei folate transport protein (18 kDa) was treated with gamma-F-MTX that had been activated with N-hydroxysuccinimide (NHS), the protein was readily visualized as a fluorescent band on SDS-PAGE electrophoretograms. The probe was also able to detect the transporter in membranes.(ABSTRACT TRUNCATED AT 250 WORDS)

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Platinum-folate compounds: synthesis, properties and biological activity

Vitols

Montejano

Duffy

et al. 1987

Advances in Enzyme Regulation

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Κ.S. Vitols

Studies on ferrochelatase. The effects of thiols and other factors on the determination of activity

Carboxypeptidase-mediated release of methotrexate from methotrexate .alpha.-peptides

The Reduction of Folate by Borohydride^*

Affinity labeling of folate transport proteins with the N-hydroxysuccinimide ester of .gamma.-isomer of fluorescein-methotrexate

Platinum-folate compounds: synthesis, properties and biological activity

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Κ.S. Vitols

Studies on ferrochelatase. The effects of thiols and other factors on the determination of activity

Carboxypeptidase-mediated release of methotrexate from methotrexate .alpha.-peptides

The Reduction of Folate by Borohydride*

Affinity labeling of folate transport proteins with the N-hydroxysuccinimide ester of .gamma.-isomer of fluorescein-methotrexate

Platinum-folate compounds: synthesis, properties and biological activity

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Product

Resources

About

The Reduction of Folate by Borohydride^*