Single-chain variable fragment: Difference between revisions

''Divalent'' (or ''bivalent'') single-chain variable fragments (di-scFvs, bi-scFvs) can be engineered by linking two scFvs. This can be done by producing a single peptide chain with two V_H and two V_L regions, yielding ''tandem scFvs''.<ref>{{cite journal|title=Development of tumor targeting anti-MUC-1 multimer: effects of di-scFv unpaired cysteine ___location on PEGylation and tumor binding|first5=SJ|last5=Denardo|first4=GL|last4=Denardo|first3=XB|last3=Shi|first2=A|last2=Natarajan |last1=Xiong|first1=Cheng-Yi|journal=Protein Engineering Design and Selection|year=2006|volume=19|issue=8|pmid=16760193|pages=359–367|url=http://peds.oxfordjournals.org/cgi/content/full/19/8/359|doi=10.1093/protein/gzl020|doi-access=free}}</ref><ref>{{cite journal|title=A revival of bispecific antibodies|first1=Peter|last1=Kufer|first2=Ralf|last2=Lutterbüse|first3=Patrick A.|last3=Baeuerle|journal=Trends in Biotechnology|volume=22|issue=5|pages=238–244|year=2004|url=http://www.micromet.de/fileadmin/template/main/pdf/publications_147881aaf61df52304237f0ee7f0cf2a.pdf|doi=10.1016/j.tibtech.2004.03.006|pmid=15109810}}</ref> Another possibility is the creation of scFvs with linker peptides that are too short for the two variable regions to fold together (about five amino acids), forcing scFvs to dimerize. This type is known as ''diabodies''.<ref>{{cite journal|pmid=8341653|title="Diabodies": small bivalent and bispecific antibody fragments|last1=Hollinger|first1=Philipp|volume=90|issue=14|pmc=46948|date=July 1993|pages=6444–8|last2=Prospero|first2=T|last3=Winter|first3=G|journal=Proceedings of the National Academy of Sciences of the United States of America|doi=10.1073/pnas.90.14.6444|bibcode=1993PNAS...90.6444H}}</ref> Diabodies have been shown to have [[dissociation constant]]s up to 40-fold lower than corresponding scFvs, meaning that they have a much higher [[affinity (pharmacology)|affinity]] to their target. Consequently, diabody drugs could be dosed much lower than other therapeutic antibodies and are capable of highly specific targeting of tumors in vivo.<ref name="Adams">{{cite journal|pmid=9652755|year=1998|last1=Adams|first1=GP|last2=Schier|first2=R|last3=McCall|first3=AM|last4=Crawford|first4=RS|last5=Wolf|first5=EJ|last6=Weiner|first6=LM|last7=Marks|first7=JD|title=Prolonged in vivo tumour retention of a human diabody targeting the extracellular ___domain of human HER2/neu|volume=77|issue=9|pages=1405–12|pmc=2150193|journal=British Journal of Cancer|doi=10.1038/bjc.1998.233}}</ref> Still shorter linkers (one or two amino acids) lead to the formation of trimers, so-called ''triabodies'' or ''tribodies''. ''Tetrabodies'' have also been produced. They exhibit an even higher affinity to their targets than diabodies.<ref>{{cite journal|title=Di-, tri- and tetrameric single chain Fv antibody fragments against human CD19: effect of valency on cell binding|first4=M|last4=Little|first3=G|last3=Moldenhauer|journal=FEBS Letters|first2=SM|volume=453|last2=Kipriyanov|issue=1|pages=164–168|first1=F.|last1=Le Gall|pmid=10403395|doi=10.1016/S0014-5793(99)00713-9|year=1999|s2cid=20213440|doi-access=free}}</ref>