Characterization of antibody-mediated inhibition of natural killer (NK) cytotoxicity: Evidence for blocking of both recognition and lethal hit stages of cytolysis

Rat antisera prepared against murine, periodate-activated alloimmune cytotoxic lymphocytes (termed RAT¹) have previously been shown to effectively block T-cell-mediated cytotoxicity (CMC) at the “lethal hit” stage of cytolysis (J. C. Hiserodt and B. Bonavida, J. Immunol.126, 256, 1981). Both natural killer (NK) and cytotoxic T lymphocytes (CTL) have been shown to mediate lysis by the same pathway, namely binding of effector to target cells, programming for lysis, and killer cell-independent target cell lysis. This result suggested that the molecular mechanism of NKCMC and CTLCMC may also be similar. In this context, RAT¹-mediated blocking of CTL was examined for its ability to block NKCMC. The results show that (1) addition of RAT¹ serum or IgG fractions blocked NKCMC in the absence of complement in a 4-hr ⁵¹Cr-release assay, and blocking was directed at the effector cell; (2) at the single-cell level, RAT¹ serum blocked the formation of conjugates between effector and target cells; (3) in a Ca²⁺-pulse experiment, in which the effectors and targets were first allowed to bind in the absence of Ca²⁺ for 1 hr at 37 °C, followed by the addition of Ca²⁺ to initiate the lytic event, RAT¹ was capable of blocking cytotoxicity after conjugate formation at the Ca²⁺-dependent lethal hit stage of cytolysis. The similarity of results in RAT¹ blocking experiments of both the CTL and NK systems suggests a common molecular mechanism of cytolysis.