A chemotactic protein for polymorphonuclear leukocytes (lung carcinoma-derived chemotaxin [LUCT]) was purified from culture fluid of the human lung giant cell carcinoma LU65C cells to electrophoretically homogeneous form through five sequential purification steps: DEAE-Sepharose, CM-Sepharose, HPLC on carboxyl-methylated-polyvinylalcohol resin, hydrophobic, and reversed-phase. The molecular mass was determined as approximately 10 kD by SDS-PAGE and isoelectric point was 10.7. The chemotactic activity (ED50 0.75 x 10(-9) M) was sevenfold more potent than that of FMLP (5 X 10(-9) M) and comparable with that of C5a (10(-9) M). NH2-terminal amino acid sequence and amino acid composition of LUCT strongly suggest that it may be closely related to the putative protein encoded by the cDNA clone (3-10C) and almost identical with a part of sequence of the chemotactic factor derived from stimulated human leukocytes in the 6th to 32nd, but not the NH2-terminal 5 amino acids. These results indicate that the carcinoma cells produce LUCT without any added stimulant and suggest that the previously isolated chemotactic monokines may correspond to des(1-5) of LUCT in the NH2-terminal region.
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1 June 1989
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June 01 1989
Purification and partial primary sequence of a chemotactic protein for polymorphonuclear leukocytes derived from human lung giant cell carcinoma LU65C cells.
K Suzuki,
K Suzuki
Department of Antibiotics, National Institute of Health, Tokyo, Japan.
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H Miyasaka,
H Miyasaka
Department of Antibiotics, National Institute of Health, Tokyo, Japan.
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H Ota,
H Ota
Department of Antibiotics, National Institute of Health, Tokyo, Japan.
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Y Yamakawa,
Y Yamakawa
Department of Antibiotics, National Institute of Health, Tokyo, Japan.
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M Tagawa,
M Tagawa
Department of Antibiotics, National Institute of Health, Tokyo, Japan.
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A Kuramoto,
A Kuramoto
Department of Antibiotics, National Institute of Health, Tokyo, Japan.
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S Mizuno
S Mizuno
Department of Antibiotics, National Institute of Health, Tokyo, Japan.
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K Suzuki
Department of Antibiotics, National Institute of Health, Tokyo, Japan.
H Miyasaka
Department of Antibiotics, National Institute of Health, Tokyo, Japan.
H Ota
Department of Antibiotics, National Institute of Health, Tokyo, Japan.
Y Yamakawa
Department of Antibiotics, National Institute of Health, Tokyo, Japan.
M Tagawa
Department of Antibiotics, National Institute of Health, Tokyo, Japan.
A Kuramoto
Department of Antibiotics, National Institute of Health, Tokyo, Japan.
S Mizuno
Department of Antibiotics, National Institute of Health, Tokyo, Japan.
Online ISSN: 1540-9538
Print ISSN: 0022-1007
J Exp Med (1989) 169 (6): 1895–1901.
Citation
K Suzuki, H Miyasaka, H Ota, Y Yamakawa, M Tagawa, A Kuramoto, S Mizuno; Purification and partial primary sequence of a chemotactic protein for polymorphonuclear leukocytes derived from human lung giant cell carcinoma LU65C cells.. J Exp Med 1 June 1989; 169 (6): 1895–1901. doi: https://doi.org/10.1084/jem.169.6.1895
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