Comparative validation of the SP6 antibody to Ki67 in breast cancer
- Lila Zabaglo1,2,
- Janine Salter1,2,
- Helen Anderson1,2,
- Emma Quinn1,
- Margaret Hills1,
- Simone Detre1,
- Roger A'Hern3,
- Mitch Dowsett1,2
- 1Royal Marsden Hospital, London, UK
- 2Breakthrough Breast Cancer Research Centre, London, UK
- 3Institute of Cancer Research, London, UK
- Correspondence to Lila Zabaglo, Breakthrough Translational Research Team, Academic Department of Biochemistry, Royal Marsden Hospital, London SW3 6JJ, UK;
- Accepted 21 May 2010
- Published Online First 29 July 2010
Aim To compare SP6 and MIB1 antibodies for Ki67 staining in breast cancer.
Background Immunohistochemical detection of Ki67 has been widely used to assess the proliferative fraction in breast cancer. Ki67 is used prognostically and is the primary end-point for some presurgical trials. MIB1 has been the preferred antibody, but SP6 has become available, with apparently improved performance. The importance of Ki67 led us to systematically compare SP6 with MIB1.
Methods Two sets of tissue microarrays were used. These were constructed from formalin-fixed paraffin-embedded breast cancers: (i) 177 cancers with data on response to an aromatase inhibitor for advanced disease (cohort 1); (ii) 200 mainly oestrogen-receptor-positive cancers without response data (cohort 2). Twenty-eight pairs of core-cut biopsies taken before and after aromatase inhibitor treatment were also assessed (cohort 3). Stained sections were examined either visually or by using an image analysis system (Ariol).
Results There was a strong correlation between the two antibodies in all cohorts of samples scored visually (cohort 1: n=161, r=0.93, p<0.0001; cohort 2: n=194, r=0.84, p<0.0001; cohort 3: n=54, r=0.89, p<0.0001). Correlation between visual and Ariol scores was markedly better with the SP6 antibody (r=0.71 and r=0.88 for MIB1 and SP6, respectively). Ki67 related similarly with time-to-treatment failure with the two antibodies (cohort 1). Changes in Ki67 values with the two antibodies after 2 weeks of aromatase inhibitor treatment also correlated strongly.
Conclusions SP6 and MIB1 provide highly comparable measures of Ki67 that predict progression of advanced disease similarly. SP6 is substantially better suited than MIB1 to image analysis.
Funding The work was funded by The Breakthrough Breast Cancer Research Centre, The Mary-Jean Mitchell Green Foundation and the NIHR Royal Marsden Hospital Biomedical Research Centre.
Competing interests None to declare.
Provenance and peer review Not commissioned; externally peer reviewed.