The CLL4 study compared conventional chlorambucil therapy versus fludarabine - alone or in combination with cyclophosphamide - note there was no Rituximab in those days. End points were: survival, response to therapy, duration of response, toxicity and quality of life. For patients who required further treatment after relapse or second line therapy for non-responders, a second randomisation compared treatment guided by the protocol versus treatment guided by the in-vitro drug sensitivity DiSC assay.

Between 1999 and 2004, a total of 777 patients were enrolled in the trial. With follow-up of patients still continuing up to 20 years later, CLL4 has also provided an opportunity to investigate the prognostic value of a number of factors, including four genetic markers by FISH analysis, IGHV gene mutation status, beta2 microglobulin level, CD38 and ZAP-70 expression, mutation of the Notch1, SF3B1 and EGR2 genes and expression of CLLU1. Long-term data from the study have been used in an overview of international studies resulting in a robust prognostic system for CLL (CLL-IPI).

In 499 CLL4 cases they employed targeted re-sequencing of 22 genes, identifying 623 mutations. After background mutation rate correction, 11/22 genes were recurrently mutated.

Gene mutations in TP53 (with/without del(17p), termed ‘TP53ab’) and EGR2 were associated with reduced PFS. TP53aband recurrent mutations in SF3B1, NOTCH1 (+3′UTR), EGR2, RPS15, NFKBIE, BRAF, KRAS and NRAS were associated with reduced OS. Mutations in MYD88 were confined to IGHV-mutated (IGHV-M) cases, having no significant impact on OS in this subgroup of patients. TP53 mutations were associated with poor response, NOTCH1 + 3′UTR mutations were associated with death from Richter’s syndrome, whilst TP53, SF3B1, NOTCH1 + 3′UTR, KRAS and EGR2 were significantly associated with  a less than 10 year survival.

HOWEVER, remember that this data regarding survival is before most of the new targeted treatments and needs to be interpreted with caution nowadays. The main contribution of this study is in looking back at old samples and identifying common mutation information and perhaps their significance in today's therapeutic landscape.

More here; nature.com/articles/s41375-...

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Jackie