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Abstract
The chemoselectivity of halo(het)arene sulfonyl halide aminations is studied thoroughly under parallel synthesis conditions, and the scope and limitations of the method are established. It is shown that SNAr-reactive sulfonyl halides typically undergo sulfonamide synthesis at the first step; the second amination is also possible provided that the SNAr-active center has sufficient reactivity. On the contrary, sulfonyl fluorides bearing an arylating moiety undergo selective transformation at the latter reactive center under proper temperature control. Further sulfur-fluoride exchange (SuFEx) reaction is also possible, which can be especially valuable for some sulfonyl halide classes. The developed two-step parallel double amination protocol provides access to a 7-Bln synthetically tractable REAL-type chemical space (nearly 70% expected synthesis success rate).
Supplementary materials
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Figure S1.
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Structures of amines 8
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Figure S2.
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Structures of amines 11.
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Figure S3
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Structures of amines 14
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Figure S4
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Structures of amines 16
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Figure S5.
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Structures of amines 17.
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Table S1.
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Parallel synthesis of sulfonamides 9.
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Table S2.
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Parallel synthesis of sulfonamides 12.
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Table S3.
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Parallel synthesis of sulfonyl fluorides 15.
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Table S4.
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Parallel synthesis of sulfonamides 18.
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NMR
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Copies of NMR Spectra
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File Description
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Contents of the Supporting Information Files
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