Characterization of Breast Lesions with Proton MR Spectroscopy

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Characterization of Breast Lesions with Proton MR Spectroscopy

Eren D. Yeh¹

¹ Department of Radiology, Division of Breast Imaging, ACC 219, Massachusetts General Hospital and Harvard Medical School, 15 Parkman St., Boston, MA 02114.

Received May 15, 2003; accepted after revision May 15, 2003.

This article is a commentary on the preceding article by Tseet al.

Address correspondence to E. D. Yeh.

Tse et al. [1] compared breast carcinomas, benign lesions, andphyllodes tumors using proton MR spectroscopy. In addition,they evaluated the biologic functional parameters of the tumorKi-67 proliferative index, tumor angiogenesis as measured by microvesseldensity, and HER2/neu oncogene overexpression. The study providesnew insight into breast carcinomas and correlation of biologic parameterswith proton MR spectroscopy.

Contrast-enhanced MRI of the breast has been shown in a numberof studies to detect breast cancers with a high degree of sensitivityranging from 95% to 100% [2]. One of the major limitations isthat false-positive enhancement occurs in benign breast lesions andcauses a relatively low specificity ranging from 37% to 97%.The combination of morphologic and dynamic enhancement curvesmay increase the sensitivity and specificity. In addition, furthercharacterization of lesions by MR spectroscopy may be usefulin improving the specificity.

MR spectroscopy of the breast is a recently described noninvasivemethod that has shown promising results in differentiating benignfrom malignant lesions. High levels of composite choline arelikely to be found in malignant lesions on proton MR spectroscopy.Low choline levels are expected in benign lesions and normalbreast tissue. The sensitivity in differentiating breast cancerfrom benign tumors of the breast has been reported to be 70–92% witha specificity ranging from 82% to 87% [3].

In their article, Tse et al. [1] address three issues: They comparethe proton MR spectroscopy results in 19 breast carcinomas froma series they reported previously with 27 cases of noncarcinomatousbreast lesions. They report on the spectroscopy results of sixphyllodes tumors, which is the largest series of phyllodes tumorsfor which in vivo proton MR spectroscopy data have been reportedto date. They correlate the results with biologic functionalparameters, which has not previously been described.

To date, at least six studies that use composite choline levelsto differentiate benign from malignant breast lesions have beenpublished. The data in the study by Tse et al. [1] confirm theprevious results. Their current article deals with 19 breastcarcinomas (18 infiltrating ductal carcinomas not otherwisespecified and one medullary carcinoma) and 21 benign breastlesions (18 fibroadenomas, one fibrocystic change, one papilloma,and one hamartoma). In addition, they analyzed six phyllodestumors, four of which were benign and two of which were of borderlinemalignancy. The proton MR spectroscopy findings were positivefor choline-containing compounds in 17 of the 19 cases of breastcancer; of the two remaining cases, one was medullary carcinomaand one was infiltrating ductal carcinoma. None of the 21 benignbreast lesions nor six phyllodes tumors showed detectable choline-containingcompounds. Therefore, the sensitivity was 89% and the specificitywas 100% in this series, similar to results previously reported.

The authors address the issue of whether biologic functionalparameters of benign and malignant lesions may affect the findingsof proton MR spectroscopy. Ki-67 antigen identifies activelyproliferating cells and correlates with higher tumor gradesand worse prognoses. In the carcinomas in this study by Tseet al. [1], the percentage of Ki-67 nuclear expression rangedfrom 0% to 45% with a mean of 17.5%, which was significantlyhigher than that in the benign lesions (range, 0–10%;mean, 1.6%) and in the phyllodes tumors (range, 0–3%;mean, 0.6%). In the two false-negative carcinomas, the Ki-67 proliferativeindex was 30% for the medullary carcinoma and 0% for the infiltratingductal carcinoma [1].

Tumors require increased vascularity for growth. Tumor angiogenesisas measured by intratumoral microvessel density correlates withprognosis in breast cancer. In this series, the mean microvesseldensity count for the carcinomas ranged from 8 to 20 (mean,13) vessels per high-power field and was significantly higherthan that of the benign lesions (range, 3.8–10.8; mean,7.4) and for the phyllodes tumors (range, 4–15; mean,7.6). The two false-negative findings of carcinoma had a similarmean microvessel density (13.4 and 11.8 vessels per high-powerfield) to the mean of the carcinoma group despite one havinga high and one having a negative Ki-67 proliferative index.This suggests that intratumoral microvessel density and intratumoralendothelial cell proliferation are independent of each other,as has been shown in a previous study [4]. In addition, thetumor angiogenesis may be unrelated to the proton MR spectroscopyresults because both false-negative findings of carcinoma hada mean microvessel density similar to that of the carcinomagroup. However, further studies with larger samples are neededbecause the number of subjects here is too small to draw anyconclusions.

The breast cancers that show HER2/neu overexpression are usually high-gradeand are associated with unfavorable prognoses. The authors found HER2/neuoverexpression in seven (36%) of the 19 patients with carcinomabut not in patients with the other lesion types including thetwo false-negative carcinomas. The authors suggest that false-negativeproton MR spectroscopy results may arise if the tumor does notoverexpress the oncogene. However, as Tse et al. [1] point out,the number of patients is too small to confirm this theory,and further work needs to be done to draw any conclusions.

One of the limitations of proton MR spectroscopy is that ithas a higher sensitivity for detection of larger malignant lesionsthan for small ones. All lesions in this series were 1.5 cmor greater in the largest linear dimension. In other seriesof proton MR spectroscopy that have been reported, the mean largestdimension of the malignant tumors was 2.0–4.9 cm [2].It is relatively easy to differentiate benign from malignantconditions in large lesions using breast MRI interpretationof morphologic and dynamic information. An adjunct method fordifferentiating malignancy would be helpful in smaller lesions, particularlythose less than 5 mm.

The sensitivity of proton MR spectroscopy of the breast maybe limited by technical factors. Most of the studies that havebeen performed to date have used 1.5-T magnets. Improvementsin the signal-to-noise ratio using higher field strength magnets,such as 3–4 T, may increase the detection of compositecholine compounds and therefore may increase the sensitivityin detection of smaller breast cancers. An additional technicalfactor that may cause incorrect sampling of the lesions andlead to false-negative results is patient motion or MRI misrepresentationof the unenhanced and enhanced images. Image misrepresentationwould be particularly troublesome for smaller lesions and couldbe alleviated by decreasing scanning times so that patientswould be less likely to move—or, ideally—by usingmethods to register the images.

The data that Tse et al. [1] present regarding phyllodes tumorssuggest that proton MR spectroscopy is not useful in differentiatingphyllodes tumors anywhere along the spectrum from benign toborderline to malignant. Phyllodes tumor should therefore be consideredin the differential diagnosis of a lesion that has a negative compositecholine signal and is therefore characterized as benign on MR spectroscopy.

Currently, proton MR spectroscopy may be useful as an adjunctto contrast-enhanced breast MRI in lesions greater than 1.5cm. Further research is needed to increase the sensitivity andspecificity of proton MR spectroscopy, particularly in differentiatingsmall (< 5 mm) benign from malignant lesions. Until technicalinnovations or further correlative data with biologic markerscan accomplish this, another potential use for proton MR spectroscopyis in monitoring locally advanced breast cancer response to treatmentwith neoadjuvant chemotherapy [5]. A comparison of the compositecholine level before treatment with subsequent choline reductionor disappearance after treatment may be a useful noninvasiveindicator of patient response to treatment.

References

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References

Tse GMK, Cheung HS, Pang L-M, et al. Characterization of lesions of the breast with proton MR spectroscopy: comparison of carcinomas, benign lesions, and phyllodes tumors. AJR2003; 181:1267 –1272[Abstract/Free Full Text]
Ore SG, Schnall MD. MR imaging of the breast for the detection, diagnosis, and staging of breast cancer. Radiology2001; 220:13 –30[Abstract/Free Full Text]
Katz-Brull R, Liven PT, Lenkinski RE. Clinical utility of proton magnetic resonance spectroscopy in characterizing breast lesions. J Natl Cancer Inst 2002;94:1197 –1203[Abstract/Free Full Text]
Vartanian RK, Weidner N. Correlation of intratumoral endothelial cell proliferation with microvessel density (tumor angiogenesis) and tumor cell proliferation in breast carcinoma. Am J Pathol1994; 144:1188 –1194[Abstract]
Jagannathan NR, Seenu V, Kumar M. Potential of in vivo proton MR spectroscopy in the assessment of breast lesions without the use of contrast agent. Radiology2002; 223:281 –282[Free Full Text]

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