BEGIN:VCALENDAR VERSION:2.0 PRODID:-//http://www.ucmr.umu.se//NONSGML kigkonsult.se iCalcreator 2.29.29 // CALSCALE:GREGORIAN METHOD:PUBLISH UID:232df5fa-eceb-40b2-9d26-61022426ad50 X-WR-CALNAME:JCal Pro Calendar X-WR-CALDESC:Your online events calendar X-WR-TIMEZONE:Europe/Stockholm BEGIN:VTIMEZONE TZID:Europe/Stockholm BEGIN:STANDARD TZNAME:CET DTSTART:20251026T030000 TZOFFSETFROM:+0200 TZOFFSETTO:+0100 RDATE:20261025T030000 RDATE:20271031T030000 END:STANDARD BEGIN:DAYLIGHT TZNAME:CEST DTSTART:20260329T020000 TZOFFSETFROM:+0100 TZOFFSETTO:+0200 RDATE:20270328T020000 END:DAYLIGHT END:VTIMEZONE BEGIN:VEVENT UID:fcff57de413469ed91fc3ae8e8f5e4dchttp://www.ucmr.umu.se DTSTAMP:20260624T053304Z CATEGORIES:General DESCRIPTION:Medical Biochemistry and Biophysics Seminar Series\, au tumn 2012

Örjan Carlborg\, Dept. of C linical Sciences\, Division of Computational Genetics\, Swedish University of Agricultural Sciences\, Uppsala\, Sweden

'Understanding the genetic architecture of complex traits'

Place: lecture hall KB3A9\ , Lilla hörsalen\, KBC

Host: Andrei Chabes
< br />Abstract
Understanding how genes contri bute to the phenotypic variability observed in populations is a major cha llenge in biology. A common approach to dissect the genetics of complex t raits is to measure the genotype of individuals in a population at a larg e number of loci across the genome and then evaluate whether the phenotyp ic mean differs between the individuals that carry particular combination s of genetic variants\, alleles\, at either individual loci (i.e. detecti on of additive\, dominance and epigenetic effects of loci) or at multipl e loci (i.e. to detect genetic interactions or epistasis). I will here gi ve a brief introduction to this topic and illustrate the insights that ca n be gained into the genetics of complex traits using these approaches by using examples from our research in domestic animals. An alternative\, a nd promising\, strategy to identify genes involved in gene-by-gene or ge ne-by-environment interactions is to search for loci that causes a differ ence in variance (a variance heterogeneity) between genotypes. This talk will be concluded by presenting some recent work to develop theory and to ols for genome-wide mapping of individual variance-controlling loci. Empi rical findings from studies of data in Arabidopsis thaliana and < em>Saccharomyces cerevisiae will be used to illustrate the contribut ion of such loci to the genetic architecture of complex traits and the im plications of the findings on our understanding of the genetic regulation of complex trait variation. DTSTART;TZID=Europe/Stockholm:20120904T151500 DTEND;TZID=Europe/Stockholm:20120904T151500 SUMMARY:Seminar - Örjan Carlborg: Understanding the genetic architecture of complex traits URL:http://www.ucmr.umu.se/about-ucmr/events/162-ucmr-calendar/165-general/ 228-seminar-oerjan-carlborg-understanding-the-genetic-architecture-of-comp lex-traits.html X-ALT-DESC;FMTTYPE=TEXT/HTML:Medical Biochemistry and Biophysics Se minar Series\, autumn 2012

Örjan Carlborg\, Dept. of Clinical Sciences\, Division of Computational Genetics\, S wedish University of Agricultural Sciences\, Uppsala\, Sweden

< strong>'Understanding the genetic architecture of co mplex traits'

Place: le cture hall KB3A9\, Lilla hörsalen\, KBC

Host: Andrei Chabes

Abstract
Understanding how genes contribute to the phenotypic variability observed in populatio ns is a major challenge in biology. A common approach to dissect the gene tics of complex traits is to measure the genotype of individuals in a pop ulation at a large number of loci across the genome and then evaluate whe ther the phenotypic mean differs between the individuals that carry parti cular combinations of genetic variants\, alleles\, at either individual l oci (i.e. detection of additive\, dominance and epigenetic effects of lo ci) or at multiple loci (i.e. to detect genetic interactions or epistasis ). I will here give a brief introduction to this topic and illustrate the insights that can be gained into the genetics of complex traits using th ese approaches by using examples from our research in domestic animals. A n alternative\, and promising\, strategy to identify genes involved in ge ne-by-gene or gene-by-environment interactions is to search for loci that causes a difference in variance (a variance heterogeneity) between genot ypes. This talk will be concluded by presenting some recent work to devel op theory and tools for genome-wide mapping of individual variance-contr olling loci. Empirical findings from studies of data in Arabidopsis th aliana and Saccharomyces cerevisiae will be used to illustr ate the contribution of such loci to the genetic architecture of complex traits and the implications of the findings on our understanding of the g enetic regulation of complex trait variation. END:VEVENT BEGIN:VEVENT UID:de1c647e8d2ac73ec52cc5288b324b7fhttp://www.ucmr.umu.se DTSTAMP:20260624T053304Z CATEGORIES:General DESCRIPTION:

Thesis Defence

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Pramod Kumar Rompikuntal\, Department of Molecular Biology

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'Outer membrane vesicle-mediated export of viru lence factors from Gram-negative bacteria'

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Place: Astrid Fagraeus-salen (A103)\, bldgs. 6A-L\, NUS 

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Opponent: Professor Ann-Beth Jonsson\, University of Stockholm

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Supervisor: Su n Nyunt Wai\, Department of Molecular Biology

DTSTART;TZID=Europe/Stockholm:20120907T090000 DTEND;TZID=Europe/Stockholm:20120907T113000 SUMMARY:Thesis Defence - Pramod Kumar Rompikuntal: Outer membrane vesicle-m ediated export of virulence factors from Gram-negative bacteria URL:http://www.ucmr.umu.se/about-ucmr/events/162-ucmr-calendar/165-general/ 210-thesis-defence-pramod-kumar-rompikuntal-outer-membrane-vesicle-mediate d-export-of-virulence-factors-from-gram-negative-bacteria.html X-ALT-DESC;FMTTYPE=TEXT/HTML:

Thesis Defence

\n

Pramod Kumar Rompikuntal\, Department of Molecular Bio logy

\n

'Outer membrane vesicle-mediat ed export of virulence factors from Gram-negative bacteria'

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Place: Astrid Fagrae us-salen (A103)\, bldgs. 6A-L\, NUS 

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Opponent: Pr ofessor Ann-Beth Jonsson\, University of Stockholm

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Superv isor: Sun Nyunt Wai\, Department of Molecular Biology

END:VEVENT BEGIN:VEVENT UID:d6a6e9feeb32ce7f3caed24e51d16aa6http://www.ucmr.umu.se DTSTAMP:20260624T053304Z CATEGORIES:General DESCRIPTION:The 'National and International' Seminar Series\, autum n 2012

Dr. Denise Monack\, Dept. of M icrobiology and Immunology\, Stanford University\, California\, USA
< br />'Chronic Salmonella carriage is controlled by a host regulato r of fatty acid metabolism PPARdelta'

Place: < /strong>lecture hall Betula\, bldg. 6M\, NUS-area

Host: Anders Sjösted\, Clinical Microbiology DTSTART;TZID=Europe/Stockholm:20120907T150000 DTEND;TZID=Europe/Stockholm:20120907T150000 SUMMARY:Seminar - Denise Monack: Chronic Salmonella carriage is controlled by a host regulator of fatty acid metabolism PPARdelta URL:http://www.ucmr.umu.se/about-ucmr/events/162-ucmr-calendar/165-general/ 233-seminar-denise-monack-chronic-salmonella-carriage-is-controlled-by-a-h ost-regulator-of-fatty-acid-metabolism-ppardelta.html X-ALT-DESC;FMTTYPE=TEXT/HTML:The 'National and International' Semin ar Series\, autumn 2012

Dr. Denise Monack\, Dept. of Microbiology and Immunology\, Stanford University\, Califo rnia\, USA

'Chronic Salmonella carriage is controlled b y a host regulator of fatty acid metabolism PPARdelta'

Place: lecture hall Betula\, bldg. 6M\, NUS-area
Host: Anders Sjösted\, Clinical Microbiology END:VEVENT END:VCALENDAR