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Seokjoo Chae, Ligand-receptor promiscuity enables cellular addressing

December 24, 2020 @ 1:00 pm - 2:00 pm KST

KAIST E2-1 room 3221, E2-1 building
Daejeon, Daejeon 34141 Korea, Republic of
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Speaker

Seokjoo Chae
KAIST

We will discuss about “Ligand-receptor promiscuity enables cellular addressing”, Su et al., bioRxiv (2021)

In multicellular organisms, secreted ligands selectively activate, or “address,” specific target cell populations to control cell fate decision-making and other processes. Key cell-cell communication pathways use multiple promiscuously interacting ligands and receptors, provoking the question of how addressing specificity can emerge from molecular promiscuity. To investigate this issue, we developed a general mathematical modeling framework based on the bone morphogenetic protein (BMP) pathway architecture. We find that promiscuously interacting ligand-receptor systems allow a small number of ligands, acting in combinations, to address a larger number of individual cell types, each defined by its receptor expression profile. Promiscuous systems outperform seemingly more specific one-to-one signaling architectures in addressing capacity. Combinatorial addressing extends to groups of cell types, is robust to receptor expression noise, grows more powerful with increasing receptor multiplicity, and is maximized by specific biochemical parameter relationships. Together, these results identify fundamental design principles governing cell addressing by ligand combinations.

Details

Date:
December 24, 2020
Time:
1:00 pm - 2:00 pm KST
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Organizer

Jae Kyoung Kim
Email
jaekkim@kaist.ac.kr

Venue

KAIST E2-1 room 3221
E2-1 building
Daejeon, Daejeon 34141 Korea, Republic of
+ Google Map
IBS 의생명수학그룹 Biomedical Mathematics Group
기초과학연구원 수리및계산과학연구단 의생명수학그룹
대전 유성구 엑스포로 55 (우) 34126
IBS Biomedical Mathematics Group (BIMAG)
Institute for Basic Science (IBS)
55 Expo-ro Yuseong-gu Daejeon 34126 South Korea
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