Loss of heterozygosity and microsatellite instability are rare in sporadic dedifferentiated liposarcoma: a study of 43 well-characterized cases.

[dedifferentiated liposarcoma]

Defects in mismatch repair proteins have been identified in Lynch syndrome -associated liposarcomas , as well as in rare sporadic sarcomas . However , it is unclear if mismatch repair defects have a role in sarcoma tumorigenesis . Microsatellite instability is a surrogate marker of mismatch repair defects .To determine whether sporadic dedifferentiated liposarcomas display microsatellite instability and , if so , to evaluate whether such instability differs between the lipogenic and nonlipogenic components of these tumors .The diagnoses of conventional dedifferentiated liposarcoma were confirmed by a combination of morphologic , immunophenotypic , and molecular studies . Standard fluorescence-based polymerase chain reaction , including 5 mononucleotide microsatellite markers (BAT 25 , BAT 26 , NR 21 , NR 24 , and MONO 27 ), as well as 2 pentanucleotide repeat markers (Penta C and Penta D ), was used to test for instability and loss of heterozygosity .We demonstrated only a single case (1 of 43 ) with microsatellite instability at one mononucleotide marker . No sarcomas showed high -level microsatellite instability . However , loss of heterozygosity at the pentanucleotide markers was observed in 8 of 43 cases . The presence of loss of heterozygosity was overrepresented in the nonlipogenic (dedifferentiated ) components compared with the paired lipogenic (well differentiated ) components .Mismatch repair defects do not contribute to sporadic dedifferentiated liposarcoma tumorigenesis . Whether the observed loss of heterozygosity drives tumorigenesis in liposarcoma , for example by affecting tumor suppressor or cell cycle regulator genes , remains to be determined .