{Reference Type}: Journal Article
{Title}: Monitoring changing patterns in HER2 addiction by liquid biopsy in advanced breast cancer patients.
{Author}: Giordani E;Allegretti M;Sinibaldi A;Michelotti F;Ferretti G;Ricciardi E;Ziccheddu G;Valenti F;Di Martino S;Ercolani C;Giannarelli D;Arpino G;Gori S;Omarini C;Zambelli A;Bria E;Paris I;Buglioni S;Giacomini P;Fabi A;
{Journal}: J Exp Clin Cancer Res
{Volume}: 43
{Issue}: 1
{Year}: 2024 Jun 29
暂无{DOI}: 10.1186/s13046-024-03105-9
{Abstract}: <B>BACKGROUND: </B>During targeted treatment, HER2-positive breast cancers invariably lose HER2 DNA amplification. In contrast, and interestingly, HER2 proteins may be either lost or gained. To longitudinally and systematically appreciate complex/discordant changes in HER2 DNA/protein stoichiometry, HER2 DNA copy numbers and soluble blood proteins (aHER2/sHER2) were tested in parallel, non-invasively (by liquid biopsy), and in two-dimensions, hence HER2-2D.<BR><B>METHODS: </B>aHER2 and sHER2 were assessed by digital PCR and ELISA before and after standard-of-care treatment of advanced HER2-positive breast cancer patients (n=37) with the antibody-drug conjugate (ADC) Trastuzumab-emtansine (T-DM1).<BR><B>RESULTS: </B>As expected, aHER2 was invariably suppressed by T-DM1, but this loss was surprisingly mirrored by sHER2 gain, sometimes of considerable entity, in most (30/37; 81%) patients. This unorthodox split in HER2 oncogenic dosage was supported by reciprocal aHER2/sHER2 kinetics in two representative cases, and an immunohistochemistry-high status despite copy-number-neutrality in 4/5 available post-T-DM1 tumor re-biopsies from sHER2-gain patients. Moreover, sHER2 was preferentially released by dying breast cancer cell lines treated in vitro by T-DM1. Finally, sHER2 gain was associated with a longer PFS than sHER2 loss (mean PFS 282 vs 133 days, 95% CI [210-354] vs [56-209], log-rank test p=0.047), particularly when cases (n=11) developing circulating HER2-bypass alterations during T-DM1 treatment were excluded (mean PFS 349 vs 139 days, 95% CI [255-444] vs [45-232], log-rank test p=0.009).<BR><B>CONCLUSIONS: </B>HER2 gain is adaptively selected in tumor tissues and recapitulated in blood by sHER2 gain. Possibly, an increased oncogenic dosage is beneficial to the tumor during anti-HER2 treatment with naked antibodies, but favorable to the host during treatment with a strongly cytotoxic ADC such as T-DM1. In the latter case, HER2-gain tumors may be kept transiently in check until alternative oncogenic drivers, revealed by liquid biopsy, bypass HER2. Whichever the interpretation, HER2-2D might help to tailor/prioritize anti-HER2 treatments, particularly ADCs active on aHER2-low/sHER2-low tumors.<BR><B>BACKGROUND: </B>NCT05735392 retrospectively registered on January 31, 2023 https://www.<BR><B>RESULTS: </B>gov/search?term=NCT05735392.