4.2 Article

Profiling heterogenous sizes of circulating tumor microemboli to track therapeutic resistance and prognosis in advanced gastric cancer

Journal

HUMAN CELL
Volume 34, Issue 5, Pages 1446-1454

Publisher

SPRINGER JAPAN KK
DOI: 10.1007/s13577-021-00568-2

Keywords

Gastric cancer; CTM; CTC; Resistance; Prognosis

Categories

Funding

  1. National Key R&D Program of China [2017YFC1309000, 2017YFC1308900]
  2. Project of State Key Laboratory of Radiation Medicine and Protection, Soochow University [GZK1201801]
  3. Major Program of National Natural Science Foundation of China [91959205]
  4. third round of public welfare development and reform pilot projects of Beijing Municipal Medical Research Institutes (Beijing Medical Research Institute) [2019-1]
  5. Wu Jieping Medical Foundation [320.6750.2021-02-15]
  6. China postdoctoral science funding [2019M660009]

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Circulating tumor microemboli (CTM) aggregated by >= 2 circulating tumor cells (CTCs) exhibit higher migratory ability compared to single CTCs. The heterogeneous sizes of CTM in gastric cancer patients are associated with therapeutic resistance, with CTM containing 3-4 CTCs specifically linked to resistance to chemotherapy/targeted therapy and poor prognosis. Larger CTM clusters, >= 5 CTCs, are only detected intra-therapeutically and indicate liver metastasis in HER2(+) gastric cancer patients.
Circulating tumor microemboli (CTM) aggregated by >= 2 circulating tumor cells (CTCs) are more migratory than single CTCs. Aside from the plasticity in their molecular characteristics, which have been considered tumor migration, CTM also possesses high size heterogeneity. This study, therefore, systematically investigated the heterogeneous sizes of CTM and their involvement in therapeutic resistance in 114 patients with advanced gastric cancer (GC) using a pre-established surface molecule-independent subtraction enrichment (SE)-iFISH strategy. CTM, which was pre-therapeutically detected in 33.3% of GC patients, can further form in another 34.78% of patients following chemo-/targeted therapies. The presence of CTM is relevant to liver metastasis as well as higher CTC levels (>= 5/6 mL). Further size-based profiling of GC-CTM revealed that CTM with 2 CTCs (CTM2) was the dominant subtype, accounting for 50.0% of all detected GC-CTMs. However, CTM with 3-4 CTCs (CTM3-4) specifically associates with chemo-/targeted therapeutic resistance and inferior prognosis. Patients with >= 1 CTM3-4/6 mL have shorter median progression-free survival and median overall survival. Unlike CTM2 and CTM3-4, which are detectable in pre-therapy and post-therapy, larger aggregated CTM >= 5 (CTM with >= 5 CTCs) was only intra-therapeutically detected in four HER2(+) GC patients, of which three experienced liver metastases. Obtained results suggested that the cluster size of GC-CTM should be dynamically profiled beyond pre-therapeutic whole CTM enumeration in terms of chemo-/targeted resistance or metastasis monitoring. GC-CTM3-4 could be a potential indicator of therapeutic resistance, while the dynamic presence of GC-CTM >= 5 implies liver metastasis in HER2(+) GC patients.

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