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On 3 May 2019, Magdalena Klanova from Charles University, Prague, CZ, and colleagues, published results from phase III GOYA (NCT01287741) and GALLIUM (NCT01332968) trials in Clinical Cancer Research. This exploratory analysis in patients with non-Hodgkin lymphoma (NHL) sought to investigate the potential prognostic value of natural killer cell count (NKCC) in predicting patient outcomes following anti-CD20 immunochemotherapy.
Baseline characteristic |
FL patients (GALLIUM) |
DLBCL (GOYA) |
---|---|---|
Median baseline PB NKCCs (range) |
222 (13−3327) cells/μl |
196 (5−1930) cells/μl |
Patients with low PB NKCCs n, (%) |
108 (10.2%) |
255 (19.8%) |
Germinal center B-cell like (GCB) |
Activated B-cell like (ABC) |
Unclassified |
P value |
|
---|---|---|---|---|
Median baseline PB NKCCs by DLBCL COO subtype (range) |
186 (6−1659) cells/μl |
200 (8−1930) cells/μl |
167 (7−1715) cells/μl |
- |
Low baseline PB NKCCs (less < 100 cells/μl) n, (%) |
83 (17.1%) |
37 (26.4%) |
54 (23.3%) |
0.022 |
The results of this exploratory analysis indicate that the number of PB circulating NK cells could act as a prognostic biomarker for FL or DLBCL patient outcomes and allow the development of novel combination treatment approaches tailored to the number of functional effector cells in NHL.
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