Stromal caveolin-1 levels predict early DCIS progression to invasive breast cancer
Here, we determined the possible association of stromal caveolin-1 (Cav-1) levels with DCIS recurrence and/or progression to invasive breast cancer. An initial cohort of 78 DCIS patients with follow-up data was examined. As ER-positivity was associated with recurrence, we focused our analysis on...
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Veröffentlicht in: | Cancer biology & therapy 2009-06, Vol.8 (11), p.1071-1079 |
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Zusammenfassung: | Here, we determined the possible association of stromal caveolin-1 (Cav-1) levels with
DCIS recurrence and/or progression to invasive breast cancer. An initial cohort of 78
DCIS patients with follow-up data was examined. As ER-positivity was associated with
recurrence, we focused our analysis on this subset of 56 patients. In this group, we
observed that DCIS progressed to invasive breast cancer in ~14% of the patient
population (8/56), in accordance with an expected progression rate of 12-15%. Nearly
ninety percent of DCIS patients (7/8) that underwent recurrence to invasive breast cancer
had reduced or absent levels of stromal Cav-1. Remarkably, an absence of stromal Cav-1
(score = 0) was specifically associated with early disease progression to invasive breast
cancer, with reduced time to recurrence and higher recurrence rate. All DCIS patients
with an absence of stromal Cav-1 underwent some form of recurrence (5/5) and the
majority (4/5) underwent progression to invasive breast cancer. This represents an overall
cumulative incidence rate of 100% for recurrence and 80% for progression. An absence
of stromal Cav-1 in DCIS lesions was also specifically associated with the presence of
inflammatory cells. Conversely, ninety-seven percent of ER(+) DCIS patients (35/36)
with high levels of stromal Cav-1 (score = 2) did not show any invasive recurrence over
the duration of follow-up (4-208 months), and 89% of such patients are estimated to
remain free of invasive recurrence, even after 15 years. Thus, determination of stromal
Cav-1 levels may be a useful new biomarker for guiding the treatment of ER(+) DCIS
patients. |
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ISSN: | 1538-4047 1555-8576 |
DOI: | 10.4161/cbt.8.11.8874 |