Ang SF , Zhao ZS , Lim L , Manser E .

	Figure 1. DAAM1 is localized to different regions in the cells.(A) Western analysis of DAAM1 expression in different cell lines. Total protein lysate (30 µg) were loaded per lane. (B) Domain organization of DAAM1. (C) Left: confocal images of COS-7 cell taken at different planes. Right: co-localization of DAAM1 with centrosomes in prophase (after centrosome duplication) marked by anti-γ-tubulin. White arrowheads indicate centrosomes. (D) Confocal images of U2OS and DAAM1-null H460 cells, as well as COS-7 and COS-7 cells with DAAM1 knockdown by siRNA (COS-7 + siDAAM1). Endogenous DAAM1 was detected by indirect immuno-fluorescence with anti-DAAM1 under identical conditions. (E) Full-length Flag-DAAM1 or Flag-hDia1 (in green) was expressed in COS-7 cells and co-stained for actin (red). Bars  = 10 µm.
	Figure 2. N-terminal regions of DAAM1 are involved with actin stress fibers and centrosome targeting.(A) GFP-Flag-DAAM1 (1–440) was expressed in HeLa and analyzed by confocal imaging. DAAM1 was immuno-localized with anti-GFP (in green). Cells were counter-stained with TRITC-phalloidin, anti-myosin IIA or anti-myosin IIB (red). (B) Table summarizing the localization of various DAAM1 constructs tested in this study. (C) COS-7 cells expressing DAAM1(100–350) form large filaments enriched for myosin IIB that do not colocalize with F-actin. Treatment with various acto-myosin disrupting drugs with the indicated concentration for 45 min do not abolish the presence of these fibrils. Bars  = 10 µm.
	Figure 3. Interaction of DAAM1 with Rho GTPases.(A) The design of putative Rho binding defective mutants was based on sequences in mDia1: RhoA complex [6]. An in-vitro pulldown assay was performed in which equal amounts of DAAM1-N wildtype (WT) or the GBD mutants were added to Sepharose beads loaded with GST or GST-RhoAV14. The proteins were transferred to PVDF and stained as shown. The membrane was subsequently probed as indicated (B) GFP-DAAM1-N WT or the GBD mutants were expressed in COS-7 cells and immuno-localized with anti-GFP and F-actin (TRITC-phalloidin); all three constructs show typical DAAM1 filamentous staining. Bars  = 10 µm.
	Figure 4. DAAM1 knockdown affects directed cell migration.(A) Efficacy of two different siRNA against DAAM1 in COS-7 cells by Western analysis at 24 hours and 48 hours post-transfection. (B) COS-7 cells transfected with control (Ctr) or human DAAM1 siRNA (si2318) for 48 hours were scratched and observed using time-lapse imaging for 12 hours. Tracks of individual cells are shown as colored lines. Bar  = 40 µm. (C) Wound-edge COS-7 cells subjected to GSK inhibitor (SB216763, 20 µM) and PKC inhibitor (RO-320432, 20 µM), or si2318 (40 pmol) were stained with anti-α-tubulin to visualize the microtubule network. Loss of DAAM1 was associated with random protrusions versus the more organized broad extensions in controls. Wound-edge U2OS cells subjected to siRNA treatment are shown in the bottom panel. Bar  = 10 µm. (D) Forward Golgi orientation of COS-7 cells transfected with control (Ctr) or DAAM1 siRNA (si2318 or si2832, 40 pmol) at 0 and 1 hour post-wounding. Cells were scored for Golgi re-orientation using a 120° sector centered on the nucleus as shown on the right. (E) Right: Western analysis of DAAM1 knockdown in U2OS cells. Left: Golgi re-orientation in COS-7 and U2OS cells treated with various inhibitors 1 hour before wounding. PKC inhibitor (PKCi) and GSK inhibitors (GSKi) were used as in (c). In these analyses, cells were scored for Golgi re-orientation in three separate experiments. Error bars indicate standard deviation from the mean.
	Figure 5. Stable expression of DAAM1 in U2OS cells.(A) Levels of mCherry-DAAM1 and endogenous DAAM1 in the five stable U2OS lines as determined by western analysis with anti-DAAM1. (B) Typical myosin IIB staining of the ventral membrane region for the control and mCherry-DAAM1 expressing cells. Bars  = 10 µm.
	Figure 6. Effects of stable DAAM1 expression in U2OS cells.(A) Cells stably expressing mCherry alone or mCherry-DAAM1 as shown in Fig. 5 were subjected to wound healing assays and stained with Alexa Fluor 633-phalloidin to visualize the actin fibers. Red arrows indicate the different arrangement of actin fibers at the leading edges of vector control and DAAM1-expressing cells. Red arrows indicate the lamella region largely devoid of stress fibers in controls (top panel red arrows), and the presence of prominent actin fibers instead for the DAAM1-expressing cells (lower panel). (B) Cell lines stably expressing the mCherry vector or mCherry-DAAM1 were subjected to scratch wounding (wound indicated by dotted lines) and images were acquired at 2 hour intervals over 6 hours using an Olympus IX71 microscope equipped with a 10x/0.25 Plan-APOCHROMAT lens. Images at 0 and 4 hour time points are shown here for control and the DAAM1 cell-line 3. (C) Line graph showing the reduction in wound gap over the entire course of 6 hours for the control line and DAAM1-expressing line 3. (D) Percentage of wound gap covered 2 hours after scratch is plotted for control versus three of the lines. Error bars indicate standard error of the mean (SEM) from 3 independent experiments. Asterisks indicate that difference in the measurement between the control and each DAAM1 expressing line is statistically significant with a p-value less than 0.05 (t-test). Bars  = 10 µm (unless specified).
	Figure 7. A model of DAAM1 involvement in directed cell migration.Through its effects on F-actin assembly and the propensity to associate with myosin IIB, DAAM1 can directly affect the regulation of the acto-myosin network. Its upstream activator, Disheveled, is involved with activation of other polarity proteins through Cdc42 [30]. Cdc42 and MRCK are implicated in nuclear movement via effects on the sub-nuclear acto-myosin network [28], [34]. PAR3/PAR6/aPKC and dynein maintain the centrosome in the cell centroid via their effects on microtubule organization [29]. The ability of DAAM1 to interact with RhoA and Cdc42 could be a focus of cooperativity between the two GTPases in the polarity pathway. Full arrows indicate direct interaction, dashed arrows indicate indirect interaction, and dotted arrows indicate interaction yet to be established in this pathway.

Alberts, Identification of a carboxyl-terminal diaphanous-related formin homology protein autoregulatory domain. 2001, Pubmed

Alberts, Identification of a carboxyl-terminal diaphanous-related formin homology protein autoregulatory domain. 2001, Pubmed
Aspenström, The diaphanous-related formin DAAM1 collaborates with the Rho GTPases RhoA and Cdc42, CIP4 and Src in regulating cell morphogenesis and actin dynamics. 2006, Pubmed
Bershadsky, Disruption of the Golgi apparatus by brefeldin A blocks cell polarization and inhibits directed cell migration. 1994, Pubmed
Desai, Cell polarity triggered by cell-cell adhesion via E-cadherin. 2009, Pubmed
Eng, The formin mDia regulates GSK3beta through novel PKCs to promote microtubule stabilization but not MTOC reorientation in migrating fibroblasts. 2006, Pubmed
Erickson, Mammalian Cdc42 is a brefeldin A-sensitive component of the Golgi apparatus. 1996, Pubmed
Etienne-Manneville, Cdc42 regulates GSK-3beta and adenomatous polyposis coli to control cell polarity. 2003, Pubmed
Evangelista, Bni1p, a yeast formin linking cdc42p and the actin cytoskeleton during polarized morphogenesis. 1997, Pubmed
Evangelista, Formins: signaling effectors for assembly and polarization of actin filaments. 2003, Pubmed
Gomes, Nuclear movement regulated by Cdc42, MRCK, myosin, and actin flow establishes MTOC polarization in migrating cells. 2005, Pubmed
Habas, Wnt/Frizzled activation of Rho regulates vertebrate gastrulation and requires a novel Formin homology protein Daam1. 2001, Pubmed , Xenbase
Higgs, Formin proteins: a domain-based approach. 2005, Pubmed
Ishizaki, Coordination of microtubules and the actin cytoskeleton by the Rho effector mDia1. 2001, Pubmed
Joberty, The cell-polarity protein Par6 links Par3 and atypical protein kinase C to Cdc42. 2000, Pubmed
Ju, Activation of the planar cell polarity formin DAAM1 leads to inhibition of endothelial cell proliferation, migration, and angiogenesis. 2010, Pubmed
Kolega, Asymmetric distribution of myosin IIB in migrating endothelial cells is regulated by a rho-dependent kinase and contributes to tail retraction. 2003, Pubmed
Kupfer, Polarization of the Golgi apparatus and the microtubule-organizing center in cultured fibroblasts at the edge of an experimental wound. 1982, Pubmed
Lammers, The regulation of mDia1 by autoinhibition and its release by Rho*GTP. 2005, Pubmed
Liu, Mechanism of activation of the Formin protein Daam1. 2008, Pubmed , Xenbase
Lo, Nonmuscle myosin IIb is involved in the guidance of fibroblast migration. 2004, Pubmed
Lu, Structure of the FH2 domain of Daam1: implications for formin regulation of actin assembly. 2007, Pubmed , Xenbase
Matusek, The Drosophila formin DAAM regulates the tracheal cuticle pattern through organizing the actin cytoskeleton. 2006, Pubmed
Mellor, Cell motility: Golgi signalling shapes up to ship out. 2004, Pubmed
Nezami, Structure of the autoinhibitory switch in formin mDia1. 2006, Pubmed
Otomo, Structural basis of Rho GTPase-mediated activation of the formin mDia1. 2005, Pubmed
Petersen, FH3, a domain found in formins, targets the fission yeast formin Fus1 to the projection tip during conjugation. 1998, Pubmed
Pollard, Regulation of actin filament assembly by Arp2/3 complex and formins. 2007, Pubmed
Pring, Mechanism of formin-induced nucleation of actin filaments. 2003, Pubmed
Pruyne, Role of formins in actin assembly: nucleation and barbed-end association. 2002, Pubmed
Rolo, Morphogenetic movements driving neural tube closure in Xenopus require myosin IIB. 2009, Pubmed , Xenbase
Romero, Formin is a processive motor that requires profilin to accelerate actin assembly and associated ATP hydrolysis. 2004, Pubmed
Rose, Structural and mechanistic insights into the interaction between Rho and mammalian Dia. 2005, Pubmed
Sagot, Yeast formins regulate cell polarity by controlling the assembly of actin cables. 2002, Pubmed
Sandoval, Role of microtubules in the organization and localization of the Golgi apparatus. 1984, Pubmed
Sato, Profilin is an effector for Daam1 in non-canonical Wnt signaling and is required for vertebrate gastrulation. 2006, Pubmed , Xenbase
Schlessinger, Cdc42 and noncanonical Wnt signal transduction pathways cooperate to promote cell polarity. 2007, Pubmed
Schmoranzer, Par3 and dynein associate to regulate local microtubule dynamics and centrosome orientation during migration. 2009, Pubmed
Seth, Autoinhibition regulates cellular localization and actin assembly activity of the diaphanous-related formins FRLalpha and mDia1. 2006, Pubmed
Skoglund, Convergence and extension at gastrulation require a myosin IIB-dependent cortical actin network. 2008, Pubmed , Xenbase
Skoufias, Spatial and temporal colocalization of the Golgi apparatus and microtubules rich in detyrosinated tubulin. 1990, Pubmed
Tan, A tripartite complex containing MRCK modulates lamellar actomyosin retrograde flow. 2008, Pubmed
Taniguchi, Mammalian formin fhod3 regulates actin assembly and sarcomere organization in striated muscles. 2009, Pubmed
Thyberg, Role of microtubules in the organization of the Golgi complex. 1999, Pubmed
Vicente-Manzanares, Regulation of protrusion, adhesion dynamics, and polarity by myosins IIA and IIB in migrating cells. 2007, Pubmed
Vicente-Manzanares, Segregation and activation of myosin IIB creates a rear in migrating cells. 2008, Pubmed
Wallar, The formins: active scaffolds that remodel the cytoskeleton. 2003, Pubmed
Watanabe, p140mDia, a mammalian homolog of Drosophila diaphanous, is a target protein for Rho small GTPase and is a ligand for profilin. 1997, Pubmed
Watanabe, Regulation of microtubules in cell migration. 2005, Pubmed
Wen, EB1 and APC bind to mDia to stabilize microtubules downstream of Rho and promote cell migration. 2004, Pubmed
Yamashita, Crystal structure of human DAAM1 formin homology 2 domain. 2007, Pubmed