E. M. Macdonald scite author profile

E. M. Macdonald

5Publications

89Citation Statements Received

28Citation Statements Given

How they've been cited

334

How they cite others

Affiliations

Chulalongkorn University, The University of Texas Medical Branch at Galveston, Western Infirmary

Publications

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Production of monoclonal antibodies specific for two distinct steric portions of the glycolipid ganglio-N-triosylceramide (asialo GM2).

Young¹,

Macdonald²,

Nowinski³

et al. 1979

192

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Two hybrid cell lines were prepared by the fusion of mouse myeloma cells with the spleen cells of BALB/c mice that had been immunized with the glycolipid ganglio-N-triosylceramide (asialo GM2). The specificity of the monoclonal antibodies produced by these hybridomas, one an IgM and the other an IgG3, has been defined by hemagglutination inhibition, complement fixation, and lysis of glycolipid liposomes by antibody and complement. A major determinant recognized by the IgM antibody is the nonreducing terminal N-acetylgalactosamine including the C6 primary hydroxyl group, but excluding the C2-acetamide group of N-acetylgalactosamine, because oxidation with galactose oxidase produced a structure showing only minimal cross-reaction with the IgM but replacement of the N-acetyl group with an N-n-butyryl group produced a glycolipid that reacts with IgM antibody to the same extent as with the unmodified glycoplipd. A major determinant recognized by the IgG3 antibody is the terminal N-acetylgalactosamine including the C2-acetamido group, but excluding the C6 primary hydroxyl group of N-acetylgalactosamine, because replacement of the N-acetyl group with an N-n-butyryl group produced a glycolipid that did not react with the IgG3 antibody; in striking contrast the IgG3 antibody reacted with the C6-oxidized glycolipid as well as with the native glycolipid. Neither antibody reacted significantly with any other natural glycolipids tested including several that are structurally related to asialo GM2 such as ganglioside GM2, ganglio-N-tetraosylceramide (asialo GM1), or ceramide dihexoside. These results indicated that in addition to the fine structure specificity described above both antibodies recognize the nonreducing terminal GalNAc beta 1 leads to 4Gal structure. The strict antigenic specificity of these monoclonal anti-glycolipid antibodies indicates their great potential as specific probes for cell surface studies.

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Tinea Capitis Caused by Trichophyton tonsurans

Hebert

Head

Macdonald

1985

Pediatric Dermatology

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Children with tinea capitis caused by Trichophyton tonsurans often have a lifetime of association with the organism and, in spite of intermittent therapy, as adults pass the infection to successive generations. While most current treatment regimens are directed at treating the individual patient, our study supports the need to evaluate and possibly treat all family members and their home environment.

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Exophiala jeanselmei infection in a postrenal transplant patient

Sindhuphak¹,

Macdonald²,

Head³

et al. 1985

Journal of the American Academy of Dermatology

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Superficial Phaeohyphomycosis of the Scrotum in a Patient With the Acquired Immunodeficiency Syndrome

Duvic

Lowe

Rios³

et al. 1987

Arch Dermatol

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The cotton swab technic for the culture of dermatophyte infections — its efficacy and merit

Head

Henry

Macdonald

1984

Journal of the American Academy of Dermatology

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E. M. Macdonald

Production of monoclonal antibodies specific for two distinct steric portions of the glycolipid ganglio-N-triosylceramide (asialo GM2).

Tinea Capitis Caused by Trichophyton tonsurans

Exophiala jeanselmei infection in a postrenal transplant patient

Superficial Phaeohyphomycosis of the Scrotum in a Patient With the Acquired Immunodeficiency Syndrome

The cotton swab technic for the culture of dermatophyte infections — its efficacy and merit

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