Variants with reduced virulence derived from Leishmania major after mutagen treatment

Abstract

Summary After several in vitro treatments of a virulent population of Leishmania major with the mutagen, N-methyl-N'-nitro-N-nitrosoguanidine (MNNG), five clones (vir^-) were obtained that did not produce cutaneous lesions after subcutaneous injection of 10⁶ promastigotes. All the control clones (vir⁺) obtained from the non-mutagenized parasite population produced progressive cutaneous lesions with as few as 10³ parasites. Late lesions were observed occasionally after injection of 10⁷ vir^- parasites. These late lesions appeared to result from the selection of virulent revertants, since parasites isolated from these lesions produced progressive lesions in BALB/c mice almost as readily as the control parasites. Two vir^- clones, one vir⁺ clone and one revertant clone were examined for survival in BALB/c macrophages in vitro. All clones were taken up by the macrophages and transformed into amastigotes. However, vir^- clones failed to multiply inside the macrophages. A vir^- clone was found to protect mice against a subsequent challenge with vir⁺ parasites.