“…In 2011, Schmid and co-workers showed that different ratios of allenols 298 and homopropargylic alcohols 299 could be obtained in the In-mediated Barbier-type addition of 4-hydroxypropargyl bromides 297 to D-glyceraldehyde acetonide, depending on the hydroxy protecting group type used (Scheme 80). 50 It was found that the application of substrates containing OMe, OAc, OCbz, and especially unprotected hydroxy groups, capable of coordinating to the indium center in the generated four-and six-membered chelated allenylindiums 300 and 302, respectively, led to an increase in the homopropargylic alcohol 299 ratio. On the other hand, the use of precursors bearing a hydroxy protected with the more bulky Bn and TBDPS groups, as well as propargyl bromides with no hydroxy group or with this functionality too distant to coordinate to the indium atom, delivered the regioisomeric allenols 298 in predominance as the result of participation of the standard open-chain, non-chelated propargylindium 301.…”