INVIVO TARGETING OF HODGKIN AND REED-STERNBERG CELLS OF HODGKINS-DISEASE WITH MONOCLONAL-ANTIBODY BER-H2 (CD30) - IMMUNOHISTOLOGICAL EVIDENCE

被引:42
作者
FALINI, B
FLENGHI, L
FEDELI, L
BROE, MK
BONINO, C
STEIN, H
DURKOP, H
BIGERNA, B
BARBABIETOLA, G
VENTURI, S
AVERSA, F
PIZZOLO, G
BARTOLI, A
PILERI, S
SABATTINI, E
PALUMBO, R
MARTELLI, MF
机构
[1] UNIV PERUGIA,INST HAEMATOL,I-06100 PERUGIA,ITALY
[2] UNIV PERUGIA,INST NUCL MED,I-06100 PERUGIA,ITALY
[3] UNIV PERUGIA,INST SURG,I-06100 PERUGIA,ITALY
[4] DAKO AS,GLOSTRUP,DENMARK
[5] SORIN BIOMED SPA,SALUGGIA,ITALY
[6] FREE UNIV BERLIN,INST PATHOL,W-1000 BERLIN 33,GERMANY
[7] UNIV VERONA,INST HAEMATOL,I-37100 VERONA,ITALY
[8] UNIV BOLOGNA,INST HAEMATOL,SERV PATHOL ANAT 2,I-40126 BOLOGNA,ITALY
关键词
D O I
10.1111/j.1365-2141.1992.tb04591.x
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
The ability of the Ber-H2 (CD30) monoclonal antibody (mAb) to target in vivo Hodgkin (H) and Reed-Sternberg (R-S) cells was investigated in six patients with advanced Hodgkin's disease (HD). The patients were injected with scaled-up quantities of 'cold' Ber-H2 mixed-up to a small dose of I-131-labelled Ber-H2, and in vivo binding of the antibody to H and R-S cells was assessed by immunohistological analysis of tumour biopsies and immunoscintigraphy. Only 50% of tumour sites were imaged at scintigraphy by the I-131-labelled Ber-H2. In contrast, immunohistological studies on tissue biopsies, taken 24-72 h following the mAb injection, showed that H and R-S cells in all tumour sites, including those that were not imaged by immunoscintigraphy, were specifically and strongly labelled in vivo by the injected Ber-H2, at a dose as low as 30-50 mg of antibody. In vivo binding of a single dose of Ber-H2 mAb to H and R-S cells did not result in any anti-tumour effect. The excellent in vivo targeting of H and R-S cells with the Ber-H2 mAb may have been the result of multiple favourable factors, including: (a) the restricted expression of the CD30 antigen in normal human tissues: (b) the low level of soluble CD30 in the serum of our patients; and (c) the high affinity of the Ber-H2 mAb for the CD30 molecule. The immunohistological results presented in this study provide a strong argument for using the Ber-H2 mAb as a carrier for delivering cytotoxic agents (isotopes or toxins) to neoplastic cells of HD refractory to conventional therapy.
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收藏
页码:38 / 45
页数:8
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