Percentage Insula Ribbon Infarction of >50% Identifies Patients Likely to Have Poor Clinical Outcome Despite Small DWI Infarct Volume

Discussion

This study demonstrates that DWI-PIRI of >50% independently predicts poor clinical outcome and can help identify patients with stroke likely to have poor outcome despite small admission DWI lesion volumes. Consequently, the DWI-PIRI score may help to more accurately weigh the potential risks versus benefits of advanced stroke treatments than assessment by the NIHSS score and DWI lesion volume alone.

These results are consistent with earlier studies demonstrating that insula infarcts are predictive of penumbral loss and poor clinical outcome compared with infarcts sparing the insula.^{5⇓–7,10,11} Of note, diffusion and perfusion MR imaging have been used to demonstrate that infarctions of the insula are associated with an increased percentage of mismatch loss (conversion of potentially viable neighboring penumbra into infarction).^5,7 Fink et al⁶ dichotomized patients with insula infarcts into “major” (equal to or more than two-thirds on 1 section or >50% on ≥2 sections) versus smaller “minor” insula lesions and found major insula infarct involvement to be associated with larger MCA territory infarcts and higher NIHSS scores, indicating more severe clinical deficits. In another study, Christensen et al¹⁰ showed significantly worse mRS scores at 3 months in patients with right-sided insula infarcts compared with those with left-sided infarcts or no insula involvement.

Our study further expands on these findings by the following means: 1) demonstrating the added prognostic value of DWI-PIRI of >50% in predicting clinical outcome in patients with small DWI lesion volumes, 2) developing a practical and easily reproducible DWI-PIRI scoring system, 3) applying this PIRI scoring method in a patient population with ICA terminus and/or proximal MCA occlusions, and 4) providing direct comparison of our PIRI scoring method with other important imaging and clinical markers of stroke outcome.

Specifically our results show DWI-PIRI of >50%, DWI infarct volume of >70 mL, NCCT ASPECTS, NIHSS score, CTA collateral score, and DWI motor strip score to be univariate predictors of poor clinical outcome, with DWI-PIRI of >50% and NIHSS score being the only independent predictors of poor outcome. The added predictive value of DWI-PIRI to the NIHSS score makes sense if one considers that the NIHSS is a clinical assessment measuring deficits from the infarct and ischemic penumbra. The NIHSS cannot distinguish whether clinical deficits originate from infarcted tissue or tissue at risk for infarction. The DWI-PIRI score provides a unique visual marker that adds value to the NIHSS by partly delineating the amount of clinical deficit due to infarct and by predicting infarct progression. Thus, the addition of DWI-PIRI may be a useful adjunct to the NIHSS and DWI infarct volume in helping to predict clinical outcome, particularly in patients with small DWI infarct volumes who may have a higher potential for infarct growth.

Our threshold of >50% DWI insula infarct involvement for predicting poor clinical outcome adds to the recent work of Kamalian et al,⁷ who demonstrated that >25% DWI insula infarct involvement was the strongest predictor of large mismatch loss (infarct growth) in a cohort of patients with proximal middle cerebral artery occlusions. Our observed larger threshold of >50% insula infarct involvement is likely because we assessed a different outcome measure. While Kamalian et al measured changes in lesion volumes based on follow-up scans, we indirectly assessed loss of insula and other MCA region functions as measured by the 90-day modified Rankin Scale.

The insula has long been an established marker of early MCA stroke^12,13 and has been shown to be among the brain regions most vulnerable to ischemia.¹⁴ The association between insula infarct involvement and worsened tissue and clinical outcome may be 2-fold: 1) Insula infarcts may serve as a marker for poor collateral flow throughout the greater MCA territory, and 2) infarcts of the insula may lead to autonomic system alterations that may contribute to adverse tissue outcome.

The insula is supplied almost exclusively by M2 segment MCA branches, with a small contribution from M1 insular branches in some individuals.¹⁵ The superior MCA division gives rise to branches that supply the anterior insula, whereas the inferior MCA division supplies the posterior insula. The insula is vulnerable to ischemia from proximal occlusion of the M1 MCA segment and the superior and inferior division MCA branches because there is limited possibility of recruiting pial collateral supply from the anterior or posterior cerebral arteries. An infarct due to proximal MCA occlusion that spares the insula but involves the more downstream MCA territory might be indicative of good pial collateral circulation, whereas an MCA occlusion with infarct including the insula can be a sign of insufficient collateral circulation and thus infarct growth.⁵

Another link between insula infarct and worsened outcome may be related to the role of the insula in modulation of the autonomic nervous system. Clinical and experimental investigations indicate that there is increased sympathetic nervous system activity, including increased plasma catecholamine levels, in insula infarcts.^5,16 Some of the effects of sympathetic system activation have been associated with adverse clinical or tissue outcome in cerebral ischemia. For example, an elevated norepinephrine concentration after stroke is a predictor of insula involvement and poor neurologic outcome,¹⁶ and likewise poststroke hyperglycemia occurs more often with insular infarcts and is associated with larger infarct size and poor neurologic outcome.^5,17 A recent study by Kemmling et al¹⁸ found a significant association between the development of hospital-acquired pneumonia in the setting of right hemispheric peri-insular strokes, an association that is thought to be related to autonomic modulation of the immune system.

The insula is a highly recognizable anatomic structure on cross-sectional imaging due to its distinctive location adjacent to the frontal and temporal operculum, just medial to the Sylvian fissure. Our high interobserver agreement in determining the DWI-PIRI score is in keeping with prior structural MR imaging studies that show high reproducibility for anatomic localization.¹⁹

Limitations of this study include a relatively small sample size, retrospective design, and heterogeneity of treatment. It is noteworthy that the unenhanced CT insula score was not an independent predictor of outcome in the multivariate model, when DWI was excluded and the admission NIHSS score was included. This may be secondary to both shorter time to imaging and lesser sensitivity for infarct detection, compared with DWI. Recanalization status, an established predictor of stroke outcome, was not available for a large number of our patients, thus precluding its entrance into our analysis. Our findings should be validated in a larger prospective study that adjusts for recanalization status.