Dysregulation of systemic soluble immune checkpoints in early breast cancer is attenuated following administration of neoadjuvant chemotherapy and is associated with recovery of CD27, CD28, CD40, CD80, ICOS and GITR and substantially increased levels of PD-L1, LAG-3 and TIM-3
- UPSpace Home
- →
- Health Sciences
- →
- Immunology
- →
- Research Articles (Immunology)
- →
- View Item
JavaScript is disabled for your browser. Some features of this site may not work without it.
Dysregulation of systemic soluble immune checkpoints in early breast cancer is attenuated following administration of neoadjuvant chemotherapy and is associated with recovery of CD27, CD28, CD40, CD80, ICOS and GITR and substantially increased levels of PD-L1, LAG-3 and TIM-3
Rapoport, Bernardo Leon; Steel, Helen C.; Benn, Carol A.; Nayler, Simon; Smit, Teresa; Heyman, Liezl; Theron, Annette J.; Hlatshwayo, Nomsa; Kwofie, Luyanda Laura Illicia; Meyer, P.W.A. (Pieter Willem Adriaan); Anderson, Ronald
Date:
2023-03-30
Abstract:
Neoadjuvant chemotherapy (NAC) may alter the immune landscape of patients
with early breast cancer (BC), potentially setting the scene for more effective
implementation of checkpoint-targeted immunotherapy. This issue has been
investigated in the current study in which alterations in the plasma
concentrations of 16 soluble co-stimulatory and co-inhibitory, immune
checkpoints were measured sequentially in a cohort of newly diagnosed, early
BC patients (n=72), pre-treatment, post-NAC and post-surgery using a Multiplex®
bead array platform. Relative to a group of healthy control subjects (n=45), the
median pre-treatment levels of five co-stimulatory (CD27, CD40, GITRL, ICOS,
GITR) and three co-inhibitory (TIM-3, CTLA-4, PD-L1) soluble checkpoints were
significantly lower in the BC patients vs. controls (p<0.021-p<0.0001; and
p<0.008-p<0.00001, respectively). Following NAC, the plasma levels of six
soluble co-stimulatory checkpoints (CD28, CD40, ICOS, CD27, CD80, GITR), all
involved in activation of CD8+ cytotoxic T cells, were significantly increased
(p<0.04-p<0.00001), comparable with control values and remained at these
levels post-surgery. Of the soluble co-inhibitory checkpoints, three (LAG-3, PDL1,
TIM-3) increased significantly post-NAC, reaching levels significantly greater than those of the control group. PD-1 remained unchanged, while BTLA and
CTLA-4 decreased significantly (p<0.03 and p<0.00001, respectively).
Normalization of soluble co-stimulatory immune checkpoints is seemingly
indicative of reversal of systemic immune dysregulation following administration
of NAC in early BC, while recovery of immune homeostasis may explain the
increased levels of several negative checkpoint proteins, albeit with the exceptions
of CTLA-4 and PD-1. Although a pathological complete response (pCR) was
documented in 61% of patients (mostly triple-negative BC), surprisingly, none of
the soluble immune checkpoints correlated with the pCR, either pre-treatment or
post-NAC. Nevertheless, in the case of the co-stimulatory ICMs, these novel
findings are indicative of the immune-restorative potential of NAC in early BC,
while in the case of the co-inhibitory ICMs, elevated levels of soluble PD-L1, LAG-3
and TIM-3 post-NAC underscore the augmentative immunotherapeutic promise
of targeting these molecules, either individually or in combination, as a strategy,
which may contribute to the improved management of early BC.
