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Please use this identifier to cite or link to this item: http://hdl.handle.net/20.500.12710/33435
Title: Breast Cancer-Associated Adipose Tissue Histologic Subtypes: Microscopic Characterization and Their Impact on Prognosis and Survival, Depending on Age
Authors: Fenesan Pasca, Mihaela Maria
Bogdan, Razvan George
Cosma, Andrei Alexandru
Vornicu, Vlad
Melnic, Eugen
Radu, Diana Veronica
Baran, Patricia
Crainiceanu, Zorin
Corlan, Ana Silvia
Cimpean, Anca Maria
Seropian, Peter
Cerneţchi, Olga
Cobec, Ionut Marcel
Keywords: breast cancer-associated adipose tissue (BCAAT);survival;invasion;prognosis
Issue Date: 2026
Publisher: MDPI
Citation: FENESAN PASCA, Mihaela Maria; Razvan George BOGDAN; Andrei Alexandru COSMA; Vlad VORNICU; Eugen MELNIC; Diana Veronica RADU; Patricia BARAN; Zorin CRAINICEANU; Ana Silvia CORLAN; Anca Maria CIMPEAN; Peter SEROPIAN; Olga CERNEȚCHI and Ionut Marcel COBEC. Breast Cancer-Associated Adipose Tissue Histologic Subtypes: Microscopic Characterization and Their Impact on Prognosis and Survival, Depending on Age. Cancers. Online. March 2026, Vol. 18, no. 6, p. 966. doi 10.3390/cancers18060966.
Abstract: Abstract Background/Objectives: The fundamental classification based on white, brown, pink, and beige adipose tissue morphology together with fat vacuole content released into the tumor microenvironment incompletely defines breast cancer-associated adipose tissue (BCAAT) heterogeneity and does not sufficiently explain its controversial impact on invasion, recurrence, or survival in breast cancer (BC). We aim to expand BCAAT characterization by systematically evaluating stromal cellular elements within peritumoral adipose tissue, including CD34-positive fibroblasts, smooth muscle actin (SMA)-positive myofibroblasts, inflammatory cells, and microvascular structures to define distinct BCAAT subgroups. Methods: CD34 and smooth muscle actin (SMA) double immunohistochemistry was performed on 109 BC tissue specimens from patients aged 35 to 79 years old, followed by microscopic evaluation of cellular and vascular components inside peritumor adipose tissue. Microscopic findings were then correlated to age, body mass index (BMI), lymphovascular (LVI) and perineural invasion (PnI), recurrence (R), and tertiary lymphoid structures (TLSs). Results: Four BCAAT subtypes have been identified as fibroblast-rich (FRich_BCAAT), myofibroblast-rich (MyoFRich_BCAAT), vascular-rich (VRich_BCAAT), and mixed-vascular and inflammatory-rich (VIRich_BCAAT). The FRich_BCAAT subtype predominates for the age subgroup 35 to 49 years old and is a significantly worse prognostic factor for survival (p = 0.022). For the age subgroup of 50 to 69 years old, the VIRich_BCAAT subtype significantly influences PnI (p = 0.05) but not survival (Log-rank test, z = 0.57, p = 0.57). VRich_BCAAT was significantly impactful for BC patient survival aged 70 to 75 years old (p = 0.043). BMI did not correlate with any of the BCAAT subtypes but was strongly correlated with prognostic markers for each BCAAT subtype. Conclusions: Based on immunohistochemically detected cellular and vascular components, four microscopic BCAAT subtypes were identified. Three of four BCCAT subtypes specifically affect BC patient prognosis and survival depending on age.
metadata.dc.relation.ispartof: Cancers
URI: 10.3390/cancers18060966
https://www.mdpi.com/2072-6694/18/6/966
https://repository.usmf.md/handle/20.500.12710/33435
ISSN: 2072-6694
Appears in Collections:ARTICOLE ȘTIINȚIFICE

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