47 What could be the reason for such tumor cells to resist complement-mediated cytotoxicity? This issue is not fully understood, although degradation of complement or interference
in its activation by such tumor cells have been hinted.48 Being given that cPiPP binds with hCG expressed on membranes of T-lymphoblastic leukemia MOLT-4 cells, the antibody could be employed as a vehicle for selective delivery of cytotoxic compounds to the tumor cells without affecting the normal healthy cells. Diferuloylmethane (curcumin) was used for this purpose. Curcumin is a remarkably safe compound; doses upto 8 g/day show neither side effects nor toxicity in humans.49 Curcumin blocks the cancer pathway by down-regulating the NFKB activation pathway,50 and suppression of IKBα kinase and
Akt activation.51 cPiPP was conjugated to curcumin using synthetic chemical reactions. A glycine Opaganib residue was generated on curcumin using BOC-Glycine. Trifluoroacetic acid was used to remove BOC group from the intermediate BOC-glycine-curcumin. Coupling of curcumin-glycine to exposed acidic amino acids (glutamic and aspartic acid) on the antibody was carried out by carbodiimide. The conjugate of curcumin-cPIPP killed effectively MOLT-4 T-lymphoblastic leukemia cells (Fig. 2). The killing was confirmed by both trypan blue exclusion and 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide (MTT) assays.52 Many years ago, our colleagues at Harvard Medical School brought to our notice human lung cancer (Chago) cells that expressed ectopically either hCG-α selleckchem or hCG-β subunits. Antibodies directed at these subunits inhibited the multiplication of these cells in vitro. PJ34 HCl They also prevented, in a dose-dependent manner, the establishment
of the cells as tumor in nude mouse (Fig. 3). In case antibodies were given after establishment of the tumor, they caused the necrosis of the tumor.53 A semisynthetic vaccine was developed previously against hCG.54,55 It consisted of a hetero-species dimer (HSD), the alpha subunit of ovine LH annealed non-covalently to beta subunit of hCG. HSD was conjugated to either tetanus toxoid (TT) or diphtheria toxoid (DT). The reason for using two different carriers was the experience that repeated immunization with hCGβ-TT caused a carrier-induced immune suppression to attached ligand, a phenomenon originally reported by Herzenberg et al.56 Immunization with an alternate carrier overcame such suppression of antibody response.57 The reason for replacing the previous hCGβ with the HSD in the vaccine was its superior immunogenicity.54 Furthermore, the antibodies formed had better neutralization capacity of the hCG bioactivity.58 The HSD-TT/DT vaccine went through multicentre phase I safety trials. It was well tolerated, and no side effects of significance were recorded.