少点错误 2024年07月09日
Sample Prevalence vs Global Prevalence
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文章探讨利用宏基因组测序检测基因工程病毒,提到若该系统以一定规模部署,可在特定情况前检测到。还讨论了疫情在不同地区的发展情况及相关因素对检测的影响。

🎯若系统以约150万美元/年的规模部署,可在监控的污水流域中,在0.2%的人被感染前检测到类似SARS-CoV-2的基因工程病毒产物。

🌍疫情在某些地方的发展会比其他地方更严重,如新冠最初在中国一个城市出现,这使得其他地区监控的污水流域初始患病率为零,而全球患病率大于零,此效应在疫情初期较为显著。

🚀像纽约这样高度连接的城市,人员流动大,疫情传播快,若选择这样的城市进行监控,其高连通性可能会减少样本患病率相对于全球患病率的滞后,甚至可能领先于全球患病率。

Published on July 8, 2024 9:00 PM GMT

Cross-posted from my NAONotebook. Thanks to Evan Fields and Mike McLaren for editorialfeedback on this post.

In Detecting Genetically Engineered Viruses With Metagenomic Sequencing we have:

our best guess is that if this system were deployed at the scale of approximately $1.5M/y it could detect something genetically engineered that shed like SARS-CoV-2 before 0.2% of people in the monitored sewersheds had been infected.

I want to focus on the last bit: "in the monitored sewersheds". The idea is, if a system like this is tracking wastewater from New York City, its ability to raise an alert for a new pandemic will depend on how far along that pandemic is in that particular city. This is closely related to another question: what fraction of the global population would have to be infected before it could raise an alert?

There are two main considerations pushing in opposite directions, both based on the observation that the pandemic will be farther along in some places than others:

My guess is that with a single monitored city, even the optimal one (which one is that even?) your sample prevalence will significantly lag global prevalence in most pandemics, but by carefully choosing a few cities to monitor around the world you can probably get to where it leads global prevalence. But I would love to see some research and modeling on this: qualitative intutitions don't take us very far. Specifically:

If you know of good work on these sorts of modeling questions or are interested in collaborating on them, please get in touch! My work email is jeff at securebio.org.



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基因工程病毒 疫情检测 宏基因组测序 连通性
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