miR-9 as predictor of response to Radiotherapy and Cetuximab in patients with head and neck cancers
PO-1107
Abstract
miR-9 as predictor of response to Radiotherapy and Cetuximab in patients with head and neck cancers
Authors: Giuseppe Fanetti1, Lorena Musco2, Francesca Citron2, Ilenia Segatto2, Francesco Micciché3, Irene Turturici1, Valentina Lupato4, Fabio Matrone1, Vittorio Giacomarra4, Luigi Barzan4, Giovanni Franchin1, Gustavo Baldassarre2
1Centro di Riferimento Oncologico di Aviano (CRO) IRCCS, Division of Radiation Oncology, AVIANO, Italy; 2Centro di Riferimento Oncologico di Aviano (CRO) IRCCS, Division of Molecular Oncology, AVIANO, Italy; 3Università Cattolica del Sacro Cuore, Fondazione Policlinico Universitario Agostino Gemelli, Polo Scienze Oncologiche ed Ematologiche, Division of Radiation Oncology, Rome, Italy; 4General Hospital “Santa Maria degli Angeli”, Division of Otolaryngology, Pordenone, Italy
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Purpose or Objective
Cetuximab (CTX) is an anti-EGFR monoclonal antibody
and demonstrated to improve survival with respect to radiotherapy (RT) alone in
patients (pts) with head and neck squamous cell carcinoma (HNSCC). RT+CTX
resulted inferior in comparison to standard chemoradiation (CRT) in HPV+ pts and
represents an option for HNSCC pts who are unfit to standard CRT with curative
intent. Biomarkers of efficacy are lacking, resulting in many pts treated with disappointing results and
unnecessary toxicities. MicroRNA (miR) expression is altered in tumors, and
their deregulation is a useful tool to predict oncologic outcome. In HNSCC, several
miRs are differentially expressed with respect to the normal/peritumoral mucosa
and we found that a four-miR signature (miR-1, -9, -133, and -150) efficiently
identifies HNSCC pts at high risk of loco-regional recurrence. This study aims
to evaluate the role of miR-9 as biomarker of efficacy of RT+CTX in terms of relapse
free survival (RFS).
Material and Methods
We reviewed retrospectively 35 pts with HNSCC treated
at our Institutions between 2012 and 2017. Inclusion criteria were: histologic
proof of HNSCC, primary tumor originating from oropharynx (OP), hypopharynx (HP)
and larynx (L), pts treated with curative intent with a total RT dose of 70
Gray with concomitant CTX. Induction chemotherapy and surgery were allowed. Recurrent
or metastatic pts were excluded. For all pts, miR-9 was evaluated on
Paraffin-embedded samples using Droplet Digital PCR Assay (ddPCR). To evaluate
the impact of miR-9 on survival, the median of expression level was used as cut
off. After treatment,
follow up was performed every 3 months with clinical examination, fibrolaryngoscopy,
and radiologic/metabolic imaging. RFS was evaluated with Kaplan
Meyer method.
Results
Median age of the 35 pts was 65 years (range 44-81 years).
Twenty-six out of 35 pts were male (74%). Current smokers and former smokers
were 14 (40%) and 9 (26%), respectively. Alcohol abuse was found in 17 (48%)
pts. HNSCC originated from OP, HP and L in 30 (86%), 1 (3%) and 4 (11%),
respectively. HPV status was detected in 16 out of 35 pts and resulted HPV+ in
only 5 pts. TNM stage was III and IV in 14 (39%) and 21 (61%) pts,
respectively. Pts treated with RT+CTX and RT+CTX+other were 26 (74%) and 9
(26%), respectively. The cut-off of miR-9 expression was 75,819 reads: 18 (58%)
showed high levels of miR-9 expression. Complete response, Partial response and
progressive disease was assessed in 18 (48%), 11 (26%) and 6 (26%) pts,
respectively. Pts with higher miR-9 expression experienced worse PFS (p=0,0382)
with respect to pts with low miR-9 expression (fig. 1).
Conclusion
Our preliminary data
suggest that high expression of miR-9 identifies a subset of HNSCC pts with
decreased PFS after RT+CTX. Further evaluations are ongoing, in particular to
evaluate the impact of miR-9 on overall survival in this cohort and in the
subgroup of pts unfit for chemotherapy
and treated with radical RT+CTX.