Neural-network based autocontouring algorithm for intrafractional lung-tumor tracking using Linac-MR

Authors

  • Yun Jihyun,

    1. Department of Oncology, Medical Physics Division, University of Alberta, 11560 University Avenue, Edmonton, Alberta T6G 1Z2, Canada
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  • Yip Eugene,

    1. Department of Oncology, Medical Physics Division, University of Alberta, 11560 University Avenue, Edmonton, Alberta T6G 1Z2, Canada
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  • Gabos Zsolt,

    1. Department of Radiation Oncology, Cross Cancer Institute, 11560 University Avenue, Edmonton, Alberta T6G 1Z2, Canada and Department of Oncology, Radiation Oncology Division, University of Alberta, 11560 University Avenue, Edmonton, Alberta T6G 1Z2, Canada
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  • Wachowicz Keith,

    1. Department of Medical Physics, Cross Cancer Institute, 11560 University Avenue, Edmonton, Alberta T6G 1Z2, Canada and Department of Oncology, Medical Physics Division, University of Alberta, 11560 University Avenue, Edmonton, Alberta T6G 1Z2, Canada
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  • Rathee Satyapal,

    1. Department of Medical Physics, Cross Cancer Institute, 11560 University Avenue, Edmonton, Alberta T6G 1Z2, Canada and Department of Oncology, Medical Physics Division, University of Alberta, 11560 University Avenue, Edmonton, Alberta T6G 1Z2, Canada
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  • Fallone B. G.

    1. Department of Physics, University of Alberta, 11322—89 Avenue, Edmonton, Alberta T6G 2G7, Canada; Department of Medical Physics, Cross Cancer Institute, 11560 University Avenue, Edmonton, Alberta T6G 1Z2, Canada; and Department of Oncology, Medical Physics Division, University of Alberta, 11560 University Avenue, Edmonton, Alberta T6G 1Z2, Canada
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Abstract

Purpose:

To develop a neural-network based autocontouring algorithm for intrafractional lung-tumor tracking using Linac-MR and evaluate its performance with phantom and in-vivo MR images.

Methods:

An autocontouring algorithm was developed to determine both the shape and position of a lung tumor from each intrafractional MR image. A pulse-coupled neural network was implemented in the algorithm for contrast improvement of the tumor region. Prior to treatment, to initiate the algorithm, an expert user needs to contour the tumor and its maximum anticipated range of motion in pretreatment MR images. During treatment, however, the algorithm processes each intrafractional MR image and automatically generates a tumor contour without further user input. The algorithm is designed to produce a tumor contour that is the most similar to the expert's manual one. To evaluate the autocontouring algorithm in the author's Linac-MR environment which utilizes a 0.5 T MRI, a motion phantom and four lung cancer patients were imaged with 3 T MRI during normal breathing, and the image noise was degraded to reflect the image noise at 0.5 T. Each of the pseudo-0.5 T images was autocontoured using the author's algorithm. In each test image, the Dice similarity index (DSI) and Hausdorff distance (HD) between the expert's manual contour and the algorithm generated contour were calculated, and their centroid positions were compared (Δdcentroid).

Results:

The algorithm successfully contoured the shape of a moving tumor from dynamic MR images acquired every 275 ms. From the phantom study, mean DSI of 0.95–0.96, mean HD of 2.61–2.82 mm, and mean Δdcentroid of 0.68–0.93 mm were achieved. From the in-vivo study, the author's algorithm achieved mean DSI of 0.87–0.92, mean HD of 3.12–4.35 mm, as well as Δdcentroid of 1.03–1.35 mm. Autocontouring speed was less than 20 ms for each image.

Conclusions:

The authors have developed and evaluated a lung tumor autocontouring algorithm for intrafractional tumor tracking using Linac-MR. The autocontouring performance in the Linac-MR environment was evaluated using phantom and in-vivo MR images. From the in-vivo study, the author's algorithm achieved 87%–92% of contouring agreement and centroid tracking accuracy of 1.03–1.35 mm. These results demonstrate the feasibility of lung tumor autocontouring in the author's laboratory's Linac-MR environment.

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