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Stanford University · 2019. 1. 1. · We began by generating invalid sequences by sampling incorrect side effects uniformly at random. For each valid sequence x = [ti, t2, . ., t5,

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Page 1: Stanford University · 2019. 1. 1. · We began by generating invalid sequences by sampling incorrect side effects uniformly at random. For each valid sequence x = [ti, t2, . ., t5,
Page 2: Stanford University · 2019. 1. 1. · We began by generating invalid sequences by sampling incorrect side effects uniformly at random. For each valid sequence x = [ti, t2, . ., t5,
Page 3: Stanford University · 2019. 1. 1. · We began by generating invalid sequences by sampling incorrect side effects uniformly at random. For each valid sequence x = [ti, t2, . ., t5,
Page 4: Stanford University · 2019. 1. 1. · We began by generating invalid sequences by sampling incorrect side effects uniformly at random. For each valid sequence x = [ti, t2, . ., t5,
Page 5: Stanford University · 2019. 1. 1. · We began by generating invalid sequences by sampling incorrect side effects uniformly at random. For each valid sequence x = [ti, t2, . ., t5,
Page 6: Stanford University · 2019. 1. 1. · We began by generating invalid sequences by sampling incorrect side effects uniformly at random. For each valid sequence x = [ti, t2, . ., t5,
Page 7: Stanford University · 2019. 1. 1. · We began by generating invalid sequences by sampling incorrect side effects uniformly at random. For each valid sequence x = [ti, t2, . ., t5,
Page 8: Stanford University · 2019. 1. 1. · We began by generating invalid sequences by sampling incorrect side effects uniformly at random. For each valid sequence x = [ti, t2, . ., t5,
Page 9: Stanford University · 2019. 1. 1. · We began by generating invalid sequences by sampling incorrect side effects uniformly at random. For each valid sequence x = [ti, t2, . ., t5,

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