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Fig. 8. Specific developmental functions are carried out by different partnerships between interacting LIM-HOM and HOM proteins. (A) Ap function in the wing is carried out by a complex of Ap and Chip. This unit dimerises to form a tetrameric complex comprising two molecules of Ap bridged by a Chip dimer. The relative stoichiometry of the two proteins is important for the formation of these complexes. Dlmo regulates Ap function by sequestering Chip into non-functional complexes. (B) Ap-Chip complexes are also necessary for the proper development of Ap motoneurones. However, balanced amounts of Chip and Ap are not required for tetrameric complex formation indicating that the limiting factor is Ap. In addition, there is no regulation by Dlmo. (C) In the fourth tarsal segment, Ap function might be achieved by a multiprotein complex, comprising Ap, Bar and Chip proteins. Our experiments indicate that the limiting factor in the formation of functional complexes is Bar, whereas Ap and Chip are more abundant. Bar interacts with Chip but not through the OID domain. This Ap-Chip-Bar functional unit could dimerise to produce a hexamer, or could consist of a molecule of each Ap and Bar bridged by a dimer of Chip. (D) High levels of Bar expression are required for the development of the fifth tarsal segment. As loss of Chip also affects the fifth tarsal segment, it is possible that a heterodimer of Bar and Chip is the functional unit in tarsus five. This unit could dimerise to produce a tetramer. (E) Synergism between Al and Lim1 is required for pretarsal development. Lim1 and Chip interact through their LIM and LID domains, respectively, and Al is also able to interact with Chip. In addition, genetic experiments show that Chip, Al and Lim1 are required in balanced amounts, suggesting that the functional unit in the pretarsus involves these three proteins simultaneously.





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