Dr. Joseph Sinkovics still stands as a live witness who was first in the late 1960s to observe
and photograph the hitherto unknown large granular lymphocytes in his own blood which were
killing allogeneic human tumor cells in vitro and photographed both the small compact human
immune T cells and the large granular NK cells of patients as they were killing human sarcoma
and melanoma cells upon encounter in vitro (Page 289 Ref [117] Page 295 Ref [156] Page 362
Ref [611]). He has been involved in the discovery of human lymphocytes cytolytic to human
cancer cells their increase during immunotherapy with viral oncolysate vaccines and thus
leading to therapeutic infusions of autologous immune lymphocytes in the 1970s to 2006 (Page
350 Ref [530] Page 358 Ref [582]). It occurs to him now to ask how those ligands evolved that
kill immune T lymphocytes by activating their PD-1 receptors (Page 368 Ref [635]). When
low-branching single-celled eukaryotes (amoeba giardia trichomonads theileria) transformed
from free-living animal cells to be the parasites of large multicellular hosts with highly
developed immune systems (including Homo) then these organisms needed those ligands to kill
immune lymphocytes of their new hosts. If so they carry the ancestors of those genes that
encode the armada of these ligands in the human genome. How the theileria convert and lyse
their bovine hosts' lymphocytes (Page 369 Ref [637])! Its ancestors must have acquired genes to
generate those ligands. Could anti-ligand mcab therapy applied for the treatment of parasitic
infestations? How the triploblastic bilateral hosts (Homo) in their malignant cells acquired
genes for those ligands: by vertical inheritance (where from?) or through lateral (horizontal)
gene transfers from ancient parasites (Page 365 Ref [619] Page 367 Ref [629 630] Page 369 Ref
[637]). There should be a short time allowed for Sinkovics to speculate about that!Thank you.