AussieNeilPartnerAdministrator• in reply toHAIRBEAR_UK11 years ago

I stand corrected thanks Nick!

From the parent posting link 2:

"TLS is most common in aggressive, fast growing (high grade) lymphomas and acute leukemias (e.g. ALL), but is less common in indolent disease such as chronic lymphocytic leukemia (CLL)."

A related posting to link 2 in the parent:

biotechstrategyblog.com/201...

includes:

"At the recent 2013 AACR annual meeting, Rod Humerickhouse, MD, PhD from AbbVie Global Pharma R&D ... told the AACR audience that Tumor Lysis Syndrome (TLS) adverse events occurred in 9 out of the 74 patients enrolled in three ABT-199 CLL clinical trials.

Two CLL trial participants died from TLS, and one had acute renal failure." (There were three trials suspended, two were for CLL and one for NHL patients.)

"Whether the tragic deaths should have been avoided we may never know, there remain unanswered questions as to whether the dose escalation was too aggressive, whether the risk of TLS was known, and if so whether patients were properly monitored."

The ABT-199 protocol now needs some adjustments to reduce the risk of TLS, arguably because ATB-199 is so effective.

From the parent posting link 2, TLS also happened on the CAR-T trials for CLL but was delayed until 20-50 days post infusion!

Chaya has more on how to prevent TLS:

updates.clltopics.org/278-p...

This just goes to show how the unlikely can still prove fatal on trials, why it is important to follow a careful expansion of trial recruits as more experience is gained with new treatment protocols and why risk reduces, but never disappears - even when the treatment becomes mainstream. Makes you appreciate how brave those entering trials - particularly in the early phases, really are and perhaps the older treatments less scary.

Neil