Role of the oral and gut microbiota as a biomarker in locoregionally advanced oropharyngeal squamous cell carcinoma (ROMA LA-OPSCC).

M. Oliva Bernal; Pierre H. H. Schneeberger; Rachel Taylor; Victor Rey; Aaron R. Hansen; Kirsty Taylor; Andrew Bayley; Andrew Hope; Ali Hosni; Scott V. Bratman; Jolie Ringash; Ralph Gilbert; Ilan Weinreb; Bayardo Perez‐Ordoñez; John Waldron; Wei Xu; David S. Guttman; Lillian L. Siu; Bryan Coburn; Anna Spreafico

doi:10.1200/jco.2019.37.15_suppl.6045

Role of the oral and gut microbiota as a biomarker in locoregionally advanced oropharyngeal squamous cell carcinoma (ROMA LA-OPSCC).

M. Oliva Bernal(University of Toronto), Pierre H. H. Schneeberger(University Health Network), Rachel Taylor(Princess Margaret Cancer Centre), Victor Rey(University Health Network), Aaron R. Hansen(Princess Margaret Cancer Centre), Kirsty Taylor(Princess Margaret Cancer Centre), Andrew Bayley(University Health Network), Andrew Hope(Princess Margaret Cancer Centre), Ali Hosni(Princess Margaret Cancer Centre), Scott V. Bratman(Princess Margaret Cancer Centre), Jolie Ringash(Princess Margaret Cancer Centre), Ralph Gilbert(Princess Margaret Cancer Centre), Ilan Weinreb(Princess Margaret Cancer Centre), Bayardo Perez‐Ordoñez(University Health Network), John Waldron(University Health Network), Wei Xu(Princess Margaret Cancer Centre), David S. Guttman(University of Toronto), Lillian L. Siu(University of Toronto), Bryan Coburn(University Health Network), Anna Spreafico(Princess Margaret Cancer Centre)

Journal of Clinical Oncology

May 20, 2019

10.1200/jco.2019.37.15_suppl.6045

Cited by 8

Abstract

6045 Background: The ROMA LA-OPSCC ( NCT03759730) study prospectively evaluated the oral and gut microbiota in a single-centre cohort of LA-OPSCC patients (pts) receiving chemoradiotherapy (CRT). Methods: LA-OPSCC pts treated with definitive CRT (IMRT plus single-agent cisplatin) were eligible. Oral swabs over the tumor site and stool samples were collected at baseline and end of CRT (EOT). Taxonomic profiles were generated by 16S rRNA sequencing. ANOSIM/Kruskal-Wallis tests were used to identify differences between baseline and EOT samples. Results: A total of 96 samples were collected from 24 evaluable pts (100% compliance). Baseline characteristics: median age = 61 (range, 50-71); smoking status current/former/never = 5/11/8; HPV+/- = 23/1; stage I/II/III/IVA = 7/7/9/1; use of antibiotics = 12 pts. In oral swabs, decreased Shannon diversity ( p< 0.01) and changes in abundance (adjusted p value: q< 0.05) of multiple taxa including Prevotella, Veillonella, and Streptococcuswere observed at EOT vs baseline. Stool diversity did not differ between baseline and EOT ( p= 0.42), but abundance of Ruminoccocus and Roseburia decreased ( q< 0.05). CRT-associated changes remained significant when controlled for stage, smoking, antibiotics, cisplatin dose and mucositis grade ( p< 0.01). In HPV+ pts, stage I-II baseline oral swabs had higher relative abundance of Clostridium IV ( p= 0.02) and Escherichia ( p= 0.04) than stage III, which had higher Fusobacterium ( p =0.03) and Gemella ( p< 0.01). Relative abundance of Actinobacteria (p < 0.01), Proteobacteria (p < 0.01) and Firmicutes (p = 0.03) was higher in stool from stage III pts . Akkermansia muciniphila was present in 57% of the stage I-II stool samples, and 11% in stage III ( p= 0.04). Conclusions: CRT in LA-OPSCC is associated with increases in potentially pathogenic genera in the oropharynx. HPV+ stage III disease was associated with higher Fusobacterium in the oropharynx, which has been implicated in tumor metastases, and with decreased prevalence of the immunotherapy-response-associated species Akkermansia in stool. These preliminary observations suggest an opportunity for the evaluation of IO based therapies or manipulation of the gut microbiota in this patient population. Clinical trial information: NCT03759730.

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