Cytokines regulate interactions between cells of the hemapoietic system

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Cytokines regulate interactions between cells of the hemapoietic system Some well-known cytokines: Erythropoietin (Epo) G-CSF Thrombopoietin IL-2 INF thrombopoietin Abbas et al. Cellular & Molecular Immunology

Interferons are cytokines that signal defense against pathogens Interferons are a group of secreted cytokines: IFN-a, IFN-b, IFN-g, etc. Released by cells in response to pathogens, including viruses and bacteria. Activate natural killer (NK) cells, which kill host cells infected with virus. IFN-a induces rapid (15-30 minutes) transcription of target genes. Induction can be 50-fold. Occurs in absence of protein synthesis (cycloheximide), implying a latent, preexisting activator. ISRE=interferon-stimulated response element Ivashkiv & Donlin (2014) Nat Rev Immunol

Nucleotide metabolism and drugs (Pyrimidines) (Purines) HPRT=HGPRT The salvage pathway allow nucleotides to be synthesized from degraded intermediates of DNA/RNA HAT selection: Aminopterin-blocks de novo pathway for purine/pyrimidine synthesis Thymidine and Hypoxanthine: substrates for salvage pathway for purine/pyrimidine synthesis Normals cells survive in HAT; HPRT- cells die in HAT 6-TG (thioguanine) is metabolized through salvage (HPRT) pathway; feedback inhibition of de novo pathway and incorporation into RNA/DNA account for toxicity

HAT selection is used to select for hybridomas Immortal Limited lifespan Hybridomas Immortal and HAT resistant Lodish et al, 2004

Homodimerization of EpoR by ligand Binding site 1 Epo Binding site 2 Each EpoR binds a distinct site on Epo Epo is not a symmetric molecule This mode of binding orients the EpoR dimer for optimal activation Syed et al (1998) Nature

Homodimerization of EpoR by ligand The natural ligand, Epo, orients the receptors in an orientation that many peptide mimics do not. Syed et al (1998) Nature

Unliganded EpoR is a preformed, cross shaped-dimer EpoR once thought to be dimerized by ligand binding Livnah et al. (1999) Science 283:987

Crystal structure of EpoR bound to peptide agonist Livnah et al. (1999) Science 283:987

Probing orientations of EpoR Seubert et al. (2003) Mol Cell 12:1239

Activation of cytokine receptors by ligand 1. Receptor dimers in absence of ligand have poor kinase activity 2. Ligand binding brings JAK kinases together for crossphosphorylation of activation loop. 3. The activated JAK kinase phosphorylates the C tail of the receptor.

Src homology domains originally found in c-scr Grosios and Traxler (2003) Drugs Fut

SH2 domains bind phosphotyrosine peptides SH2 is a small, phosphotyrosinebinding domain SH2= Src homology domain 2 STAT transcription factors contain N- terminal DNA binding domain, an SH2 domain, and a C-terminal region with a tyrosine. Zhong et al. (2005) PNAS

Activated receptors recruit and activate STAT Monomeric STAT is recruited to receptor due to SH2 binding to phosphotyrosine. C-terminal tyrosine of STAT is phosphorylated. Phosphorylated STAT dissociates, homodimerizes via SH2- phosphotyrosine interactions. Dimerization exposes NLS, and STAT is imported into the nucleus. STATs activate transcriptional program.

Model for cytokine receptor activation: ligand dimerizes receptor Lodish et al, 2004

Interferon treatment induces nuclear translocation of STAT Koster & Hauser (1999). E. J. Biochem 260:137.

Downregulation of receptor activity Binding of SH2 domain of SHP1 to the activated receptor: Activates its phosphatase catalytic activity Allow it to dephosphorylate the JAK2 activation loop, inactivating the JAK kinase activity STAT5 induces SOCS protein expression in erythropoietin-stimulated erythroid progenitor cells. binds to specific phosphotyrosine residues on EpoR or JAK2, blocking binding of other signaling proteins. targets the receptor and JAK2 for degradation by the ubiquitin proteasome pathway.

Receptor tyrosine kinases Some well-known receptor tyrosine kinases: receptors for NGF, PDGF, FGF, EGF RTK s have intrinsic kinase activity that is activated by ligand-induced dimerization. Cross-phosphorylation of kinase domains at activation lip leads to conformational change and activation. Cytosolic tail of receptor is phosphorylated on tyrosines and these sites then act as docking sites for signaling proteins. (Analogous to JAK kinases and cytokine receptors)

An adapter protein and GEF link activated RTKs to Ras

An adapter protein and GEF link activated RTKs to Ras G-GDP (inactive) GAP (inhibitor) P i GEF (activator) G-GTP (active) Grb2 is an adaptor protein, linking sos to RTK. Sos activates Ras by nucleotide exchange. What is downstream of Ras?

Ras activates the MAP kinase cascade N-term regulatory domain of Raf inhibits kinase activity; this inactive conformation is stabilized by 14-3-3 protein. Ras-GTP binds Raf's N-term domain to relieve inhibition. Raf is also activated by dephosphorylation and phosphorylation events.

Haploid yeast cells can be a or a mating type Spore germination A form of asymmetric cell division, due to transport of Ash1 mrna (prevents HO transcription) to daughter cell. Switching is always to the opposite mating type Mating-type conversion in mother cell Lodish et al, 2000

The MAT locus determines mating type Silent Active Silent MAT locus encodes for cell-type specific transcription factors. As a result, a haploids, a haploids, and a/a diploids each have their own transcriptional profile. Lodish et al, 2000

Life cycle of the budding yeast, S. cerevisiae 1n 2n 2n 1n Lodish et al, 2000

Mating factors induce yeast mating Lodish et al, 2000

A MAP kinase cascade mediates signaling in the yeast mating pathway In yeast, Gab activates MAPK cascade Lodish et al, 2004

Multiple MAP kinase pathways are involved in response of yeast cells to stimuli Scaffold protein may help to keep specificity of pathways Lodish et al, 2000

Infection of cells with v-raf virus leads to activation of MAPK and MAPKK MAPKK MAPK MAPKK MAPK MAPK MAPKK EC12, 22W = Moloney mouse sarcoma viruses containing activated v-raf (N-term truncations) The three cellular Raf genes are ser/thr kinases with N-term regulatory domain. Cell lysates fractionated by ion exchange, and fractions assayed for MAPK and MAPKK activity MAPK activity: assay phosphorylation of MBP Control virus No serum: Serum: No serum No virus: EC12 virus: No serum 22W virus: MAPKK activity: assay phosphorylation of MBP through recombinant inactive MAPK Control virus expresses a more severely truncated v-raf that is inactive. Serum or v-raf is able to induce MAPKK and MAPK activity in serum-starved cells. Dent et al. (1992) Science 257:1401

Phosphorylation of activation lip activates MAP kinase In inactive state, catalytic site is blocked by lip. Phosphorylation of lip by MEK leads to binding of ATP to catalytic site and dimerization, which allow nuclear localization

Phosphorylation of MAPK leads to nuclear translocation Khokhlatchev et al (1998). Cell 93:605

Summary of mammalian MAP kinase cascade N-term regulatory domain of Raf inhibits kinase activity; this inactive conformation is stabilized by 14-3-3 protein. Ras-GTP binds Raf's N-term domain to relieve inhibition. Raf is also activated by dephosphorylation and phosphorylation events.

Phosphorylation of MAPK leads to nuclear translocation and gene activation

The R7 photoreceptor in Drosophila is used to study RTK pathways Each ommatidia is an eye that contains 20 cells (8 photoreceptors). R8 differentiates first; R7 last. In sevenless mutant, R7 has non-neuronal fate, and the fly cannot sense UV light. Mosiac analysis shows sev is required cell autonomously in R7. Nagaraj &Banerjee (2004) Int J Dev Biol Gilbert. Developmental Biology, 8 th edition Sev is a receptor tyrosine kinase; Boss is its ligand. Screens in this system identified GRB2, SOS (son of sevenless), and Ras. Boss (Bride of sevenless) mutants also lack R7, but the gene product is required in R8.

Genetic dissection of vulva development in C. elegans The gonadal anchor cells sends an inductive signal to ventral precursor cells that generate vulval tissue. The anchor cell produces Lin-3 (an EGF molecule). The precursor cells require let-23 (RTK) and Ras (let-60) for vulva devlopment. Moghal & Sternberg (2003) Exp Cell Res

The MAPK casade in vulva development Moghal & Sternberg (2003) Exp Cell Res