THE MECHANISM OF ANTIGENIC STIMULATION OF PRIMARY AND SECONDARY CLONAL PRECURSOR CELLS

doi:10.1084/jem.136.2.241

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ARTICLE

THE MECHANISM OF ANTIGENIC STIMULATION OF PRIMARY AND SECONDARY CLONAL PRECURSOR CELLS

Norman R. Klinman ¹

¹ From the Department of Microbiology, University of Pennsylvania School of Medicine, Philadelphia, Pennsylvania 19104

Cell transfers to carrier-immunized irradiated mice have permittedan analysis of the in vitro stimulation of clonal precursorsof anti-2,4-dinitrophenyl (DNP) antibody-producing cells derivedfrom both immune and nonimmune mice. The results indicate that:(a) carrier-specific enhancement is obligatory for stimulationof primary precursor cells and increases both the size and numberof detectable foci derived from secondary precursors. (b) Thiscarrier-specific enhancement is most apparent in the stimulationof precursors of high-affinity antibody producer cells. (c)The antibody produced by primary foci, like that of secondaryfoci, appears homogeneous. (d) The frequency of clonal precursorsin normal spleens is 38% that in spleens from mice 4–8months after immunization, and the number of such precursorsin normal spleens can be reduced fivefold by specific suppressionof donor mice with soluble antigen. (e) The average of associationconstants of primary monofocal antibodies, like that of primaryserum antibody produced in carrier-primed mice, is less than10-fold lower than that of secondary clonal or serum antibody.(f) The affinity of primary monofocal antibodies shows a slightdependence on stimulating antigen concentration; however, aminimum threshold affinity consonant with stimulation is apparent.(g) Free hapten inhibits antigenic stimulation of primary precursorcells at a much lower concentration than is required for theinhibition of secondary precursors.

These results are interpretedas indicating that (a) primary stimulation, like secondary stimulation,results from the selective stimulation by antigen of a populationof cells differing from one another in their potential antibodyproduct but each having only a single such product; (b) theantigen receptors of primary cells interact with antigen asif they are monovalent while receptors of secondary cells evidencemultivalence; (c) antigenic stimulation appears to require botha relatively high affinity of receptors for bound antigen andan interlinking of receptors through such antigen; stimulationis thus seen as resulting from a stabilization of receptorswithin antigen-receptor aggregates to the cell surface; (d)T-cells appear to serve both in cross-linking antigens and inamplifying the size of stimulated clones.

Submitted on April 12, 1972

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