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Ramanujan Hegde (MRC) 2: Quality Control of Protein Localization 

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www.ibiology.org/cell-biology...
Part 1: Compartmentalization of Proteins Inside Cells: Hegde reviews key historical experiments that have informed our understanding protein localization within a cell.
Part 2: Quality Control of Protein Localization: Mislocalization of proteins can have devastating effects for the entire organism. Hegde explains how cells detect and degrade mislocalized proteins.
Part 3: Recognition of Protein Localization Signals: How does the protein translocation machinery recognize thousands of distinct signal sequences and target proteins to cellular membranes or for secretion?
Talk Overview:
Cells are organized into many different compartments such as the cytosol, nucleus, endoplasmic reticulum (ER), and mitochondria. Almost all proteins are made in the cytosol, yet each cellular compartment requires a specific set of proteins. How does the cell regulate protein localization to be sure that proteins end up where they should? In his first lecture, Manu Hegde reviews the history of this field and highlights key experiments that have led to our current understanding of how protein localization occurs.
In his second lecture, Hegde explains that although the protein localization system usually operates accurately, it does sometimes fail. This can be due to genetic mutations, stress within an organelle, or just intrinsic inefficiencies that accompany any complex process. As a graduate student, Hegde used a cell-free in vitro system to study the translocation of prion protein into the ER. He found that a small amount of prion protein did not completely cross the ER membrane as expected, but remained in a transmembrane form. Worried that this was an artifact of the in vitro system, he designed experiments in mice to see what the effect of an increase in mislocalized, transmembrane prion protein would be. He found a striking result - even a small increase in the amount of transmembrane prion protein caused increased neurodegeneration in mice. It turns out that incomplete translocation is not unique to prion protein. Hegde tells us how, as an independent investigator, his lab went on to investigate why this happens and how the cell monitors and degrades proteins that are not properly localized.
Proteins that are secreted from the cell or localized to the plasma membrane need first to be translocated into the lumen of the ER or inserted into the ER membrane. Thousands of proteins, each with a unique signal sequence, move through this pathway. How does the protein translocation machinery recognize these diverse signals and correctly localize the protein? In his third talk, Hegde describes studies from his lab using cryo-electron microscopy to visualize the translocation machinery at different stages in the recognition and engagement of a secreted or membrane inserted protein. The structural information gleaned from these experiments helps to explain how the protein translocation machinery works with high fidelity even when it needs to recognize diverse signal sequences.
Speaker Biography:
As an undergraduate, Ramanujan (Manu) Hegde studied biology at the University of Chicago with the thought that he would become a doctor. His summers and spare time were spent working in a lab, where he came to love the problem-solving of basic research. Hegde then fled Chicago winters for the sunshine of The University of California, San Francisco, where he completed an MD-PhD combined degree program. By then, he had decided to pursue basic research as a career, and moved to the National Institutes of Health where he was an investigator for 11 years. In 2011, Hegde moved to the Laboratory of Molecular Biology in Cambridge, England, where his research focuses on the mechanisms of protein biosynthesis and quality control.
Hegde’s research contributions have been recognized with his election as a member of the European Molecular Biology Organization in 2013 and as a Fellow of the Royal Society in 2016.
Learn more about Manu Hegde’s research here:
www2.mrc-lmb.cam.ac.uk/groups/...
and
www2.mrc-lmb.cam.ac.uk/group-l...

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26 июл 2024

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Комментарии : 6   
@raymondrupp549
@raymondrupp549 7 лет назад
thank you for clearly and concisely explaining this exciting subject. you are a master teacher.
@Gabysa1
@Gabysa1 6 лет назад
Thanks for the explanation! At University my Professor explained just the mechanism of protein localization, and I studied without understanding a lot. Is so interesting to know the different approches used to understand this cellular mechanism. Thanks again!!!
@tactileslut
@tactileslut 4 года назад
Love it! Fails the test, starts his own lab and proves the test wrong, even without modern gene printing magic.
@woloabel
@woloabel Год назад
(On Tuesday of April 18, 2023). ON the Matter of GMOs and PhD Ramanujan Hegde (MRC) and Quality Control of Protein Localization: 1) Endoplasmic Reticulum Stress-Associated Proteins and ER Associated Degradation (ERAD) certainly must be flawed in Pathology of Deposition (Tau Proteins, Amyloid Plaques) and Neurodegeneration is Perhaps the Most Preventable Disease Process of Geriatrics, for Alzheimer's Onset is late Age and its Morbidity is the only Limiting Factor where Death mainly ensues by this Inefficacious and Overburden Metabolism of Pathological Protein Biosynthesis. Certainly, the understanding of this Process Homeostatically will yield results of Vast Pharmacotherapeutics (I almost already sense Enzyme Proteomics of Recombinant DNA Technology alleviating this Pathology slightly). Prions (PrP) Disease and the awful Process of Proteins being Aetiologic Agents of Infectivity has to be an Idiopathic Process while Science helplessly concerns it efforts in Spreads or in trivial Investigations of Pathway Modulation (Carcinogenesis and Autophagy) or even Metabolism Alteration (GLP-1 Memetics and the Stupefaction of Mediating Diabetes) when essentially Pathology Recognition and Re-Envisionment is Primary and Wanting. I mean what is to be understood in a Hormone Pathological Milieu of Self-Destruction, ie Contraception via Estrogen Intake or the Gluttonous Monosaccharidosis of Diabetes Mellitus Insulin Resistence or worse yet treating a Psychosis as if was simply a Metabopathy. 2) I do feel this Investigation, as lethargic and Ill-funded it might be, is Meritorious (Protein Localization) in just about in every way important (Geriatrics, Primary Care Medicine of Prophylaxis) and even the Crux of My Inquisition, Metabolic Inherited Diathesis--Progeria And the Inevitability to even Develop let alone Prosper is serious Pathology. I make all efforts and Means to Remediate the Nature's Curse while abstain absolutely in the Disease Profiteering or Mediation (Symptomatic Costly Remediation is far from Humanism's Value or Ideal therein). While therapies of dubious and reckless Expenditure HAART, Statin Therapy, Hyperglycemic Controls are active areas of Science, they too are as flawed in Means and Ends as Making Antibiotics for Hyper-antibiolgicals, that is over reliance on Chemotherapy of Antibiotics. This is not only Breeding Antibiotic Resistance but also Biohazardous Live Matter--Walking, Talking Biological Warefare is not either a Right or a Peaceful Sound Approach to Infectious Disease. PhD Ramanujan Hedge, es muss haben gewessen besser aber heute wir werden sehen Apokalpse der Endmannschafts. Heil!
@hitkarshkushwaha2434
@hitkarshkushwaha2434 3 года назад
Sir, i want to join your lab... I Iove molecular biology
@hraqhraq
@hraqhraq 3 года назад
I felt sorry for the ataxic mouse
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