Could Filtering Our Aged Blood Keep us Young? – Article by Steve Hill and Nicola BagalĂ
Steve Hill
Nicola BagalĂ
Editorâs Note: In this article, Mr. Nicola BagalĂ and Steve Hill present the interview they conducted with Dr. Irina Conboy of Berkeley University and Dr. Michael Conboy of Havard University on the topic of youthful blood. This article was originally published by the Life Extension Advocacy Foundation (LEAF).
                  ~ Kenneth Alum, Director of Publication, U.S. Transhumanist Party, February 17, 2018
Due to a recently published study on the effects of young plasma on aged mice, we got in touch with Dr. Irina Conboy of Berkeley University. Dr. Conboy is an Associate Professor at the Department of Bioengineering and an expert in stem cell niche engineering, tissue repair, stem cell aging and rejuvenation. Before we dive into the main topic, letâs familiarize ourselves a little with Dr. Conboy and her work.
Dr. Conboy got her Ph.D. at Stanford University, focusing on autoimmunity. She met her partner in scienceâand in lifeâDr. Michael Conboy at Harvard and they got married before embarking on graduate studies; they celebrated their Silver Anniversary a few years ago. During her postdoctoral studies, she began focusing on muscle stem cells, trying to figure out what directs them to make new healthy tissue and what causes them to lose their ability to regenerate the tissues they reside in as we age [1].
Together with her husband Michael, she eventually discovered that old stem cells could be reactivated and made to behave like young ones if appropriately stimulated. The Conboysâ parabiosis experimentsâwhich consisted in hooking up the circulatory systems of aged and young miceâshowed that old age is not set in stone and can be reversed in a matter of weeks [2].
The follow-up work by the Conboys uncovered that age-accumulated proteins, such as TGF-β1, inhibited stem cellsâ ability to repair tissues even in young mice, and when TGF-β1 signaling is normalized to its young levels, old mice (equivalent to 80-year old people) have youthful muscle regeneration and better neurogenesis in the hippocampus (the area of the brain that is responsible for memory and learning) [3].
While young blood did appear to be beneficial to old stem cells, their evidence suggested that the real culprit of the broad loss of tissue repair with age was the negative influence of age-accumulated inhibitory proteins in aged tissues and circulation, also called the stem cell niche [4].
This conclusion is certainly compatible with the view of aging as a damage accumulation process [5]. As Irina herself pointed out in this interview, in the parabiosis experiments, the old mice had access to the more efficient young organs: lungs, liver, kidneys and immune system of the younger mice, which likely accounted for many of the benefits observed in the elderly parabiosed mice. With respect to the rejuvenation of the brain, the old mice experienced environmental enrichment by being sutured to young, more active parabionts, and this is known to improve the formation of new brain cells, learning, and memory.
An aged niche blocks the action of old and young stem cells alike very quickly; therefore, as Dr. Conboy observed in an article in the Journal of Cell Biology, we canât treat the diseases of aging by simply transplanting more stem cells, because they will just stop working. Their niche needs to be appropriately engineered as well. Fortunately, there are potential solutions to this problem; such as the use of artificial gel niches and defined pharmacology that are designed to protect transplanted or endogenous stem cells from the deleterious environment of the old body.
This research holds the potential to significantly postpone the onset of age-related diseases and possibly reverse them one day, including frailty, muscle wasting, cognitive decline, liver adiposity and metabolic failure, but Dr. Conboy remains cautious about the possibilities until more data is in. However, she does think that longer and healthier productive lives could improve peopleâs attitudes towards the environment and treating each other with compassion and respectâa view that we definitely share.
We managed to catch up with Irina and Michael Conboy and talk to them about their work.
For the sake of those new to the topic, what is it in young blood and aged blood that affects aging?
Irina: Numerous changes in the levels of proteins that together regulate cell and tissue metabolism throughout the body.
Mike: We wondered why almost every tissue and organ in the body age together and at a similar rate, and from the parabiosis and blood exchange work now think that young blood has several positive factors, and old blood accumulates several negative, âpro-agingâ factors.
A lot of media attention and funding is currently being directed to youthful blood transfusions; how can we move beyond this to potentially more promising approaches, such as filtering and calibration of aged blood?
Irina: People need to understand not just the titles, abstracts and popular highlights of research papers, but the results and whether they support (or not) the promise of rejuvenation by young blood. In contrast to vampire stories, we have no strong experimental evidence that this is true, and there is a lot of evidence that infusing your body with someone elseâs blood has severe side effects (even if it is cell-free).
Mike: Translational research!
Some evidence suggests dilution is the most likely reason that young blood has some beneficial effects; what are your thoughts on this recent study [6] in rats that shows improved hepatic function partially via the restoration of autophagy?
Irina: There are certainly âyoungâ blood factors that are beneficial, not just a dilution of the old blood, and this benefit differs from organ to organ. We have published on improved liver regeneration, reduced fibrosis and adiposity by transfusion of old mice with young blood, but these are genetically matched animals, and in people, we do not have our own identical but much younger twins [7].
If dilution is also playing a role here, then can we expect similar or better results from calibrating aged blood?
Irina: Yes, and our work in progress supports the idea.
In your 2015 paper, you identified that TGF-β1 can be either pro-youthful or pro-aging in nature, depending on its level [8]. In the study, you periodically used an Alk-5 inhibitor to reduce TGF-β1 levels and promote regeneration in various tissues. In the study, you showed that TGF-β1 was important in myogenesis and neurogenesis; is there reason to believe that this mechanism might be ubiquitous in all tissues?
Irina: Yes, because TGF-β1 receptors are present in most cells and tissues.
Also, TGF-β1 is only one of a number of factors that need to be carefully balanced in order to create a pro-youthful signalling environment. How many factors do you believe we will need to calibrate?
Irina: There will be a certain benefit from calibrating just TGF-beta 1, but also additional benefits from more than one or just TGF-beta.
How do you propose to balance this cocktail of factors in aged blood to promote a youthful tissue environment?
Irina: We are working on the NextGen blood apheresis devices to accomplish this.
So, you are adapting the plasmapheresis process to effectively âscrubâ aged blood clean and then return it to the patient. This would remove the need to transfuse blood from young people, as your own blood could be filtered and returned to you, and no immune reaction either, right?
Irina: Accurate.
This plasmapheresis technique is already approved by the FDA, we believe, so this should help you to develop your project faster, right?
Irina: Exactly.
Do you think a small molecule approach is a viable and, more importantly, a logistically practical approach to calibrate all these factors compared to filtering aged blood?
Irina: Yes, it is a very feasible alternative to the NextGen apheresis that we are working and publishing on.
It is thought that altered signaling is caused by other aging hallmarks higher up in the chain of events; even if we can âscrubâ aged blood clean, is it likely to have a long-lasting effect, or would the factors reach pro-aging levels fairly quickly again if nothing is done about the other hallmarks antagonizing them?
Irina: That needs to be established experimentally, but due to the many feedback loops at the levels of proteins, genes and epigenetics, the acquired youthful state might persist.
Ultimately, could a wearable or an implanted device that constantly filters the blood be the solution to these quickly accumulating factors?
Irina: Maybe, but the first step of a day at a NextGen apheresis clinic once every few months might be more realistic.
Filtering seems to be a far more practical solution, so how are you progressing on the road to clinical trials?
Irina: We are collaborating with Dr. Dobri Kiprov, who is a practicing blood apheresis physician with 35 years of experience, and he is interested in repositioning this treatment for alleviating age-related illnesses.
Senolytics and removing senescent cells and the resulting inflammation they cause during the aging process has become a hot topic in the last year or so. What are your thoughts on senolytics as a potential co-therapy with a blood filtering approach?
Irina: Might be good, but we should be careful, as p16 is a normal, good gene that is needed for many productive activities by many cells.
What do you think it will take for the government to fully support the push to develop rejuvenation biotechnology?
Irina: Clear understanding of the current progress and separating the real science from snake oil is very important for guiding funding toward realistic clinical translation and away from the myth and hype.
The field is making amazing progress, but, sadly, it is plagued by snake oil. As much as an âanti-aging free marketâ encourages innovation, it also encourages hucksters. How can a member of the public tell the difference between credible science and snake oil?
Irina: I was thinking for some time about starting a popularized journal club webpage where ordinary people can see what we typically critically point out in the lab setting about published papers and clinical trials.
How can our readers learn more about your work and support your research?
Irina: The new Conboy lab website is coming up; meanwhile, contact me and Dr. Mike at iconboy@berkeley.edu and conboymj@berkeley.edu
Conclusion
We would like to thank Irina and Michael for taking the time to answer our questions and for providing the readers with a fascinating insight into their work.
Literature
[1] Conboy, I. M., Conboy, M. J., Smythe, G. M., & Rando, T. A. (2003). Notch-mediated restoration of regenerative potential to aged muscle. Science, 302(5650), 1575-1577. [2] Conboy, I. M., Conboy, M. J., Wagers, A. J., Girma, E. R., Weissman, I. L., & Rando, T. A. (2005). Rejuvenation of aged progenitor cells by exposure to a young systemic environment. Nature, 433(7027), 760-764. [3] Yousef, H., Conboy, M. J., Morgenthaler, A., Schlesinger, C., Bugaj, L., Paliwal, P., ⌠& Schaffer, D. (2015). Systemic attenuation of the TGF-β pathway by a single drug simultaneously rejuvenates hippocampal neurogenesis and myogenesis in the same old mammal. Oncotarget, 6(14), 11959. [4] Rebo, J., Mehdipour, M., Gathwala, R., Causey, K., Liu, Y., Conboy, M. J., & Conboy, I. M. (2016). A single heterochronic blood exchange reveals rapid inhibition of multiple tissues by old blood. Nature communications, 7. [5] LĂłpez-OtĂn, C., Blasco, M. A., Partridge, L., Serrano, M., & Kroemer, G. (2013). The hallmarks of aging. Cell, 153(6), 1194-1217. [6] Liu, A., Guo, E., Yang, J., Yang, Y., Liu, S., Jiang, X., ⌠& Gewirtz, D. A. (2017). Young plasma reverses ageâdependent alterations in hepatic function through the restoration of autophagy. Aging cell. [7] Rebo, J., Mehdipour, M., Gathwala, R., Causey, K., Liu, Y., Conboy, M. J., & Conboy, I. M. (2016). A single heterochronic blood exchange reveals rapid inhibition of multiple tissues by old blood. Nature communications, 7. [8] Yousef, H., Conboy, M. J., Morgenthaler, A., Schlesinger, C., Bugaj, L., Paliwal, P., ⌠& Schaffer, D. (2015). Systemic attenuation of the TGF-β pathway by a single drug simultaneously rejuvenates hippocampal neurogenesis and myogenesis in the same old mammal. Oncotarget, 6(14), 11959.
About Steve Hill
As a scientific writer and a devoted advocate of healthy longevity technologies Steve has provided the community with multiple educational articles, interviews and podcasts, helping the general public to better understand aging and the means to modify its dynamics. His materials can be found at H+ Magazine, Longevity reporter, Psychology Today and Singularity Weblog. He is a co-author of the book âAging Prevention for Allâ â a guide for the general public exploring evidence-based means to extend healthy life (in press).
About Nicola BagalĂ
Nicola BagalĂ has been an enthusiastic supporter and advocate of rejuvenation science since 2011. Although his preferred approach to treating age related diseases is Aubrey de Greyâs suggested SENS platform, he is very interested in any other potential approach as well. In 2015, he launched the blog Rejuvenaction to advocate for rejuvenation and to answer common concerns that generally come with the prospect of vastly extended healthy lifespans. Originally a mathematician graduated from Helsinki University, his scientific interests range from cosmology to AI, from drawing and writing to music, and he always complains he doesnât have enough time to dedicate to all of them which is one of the reasons heâs into life extension. Heâs also a computer programmer and web developer. All the years spent learning about the science of rejuvenation have sparked his interest in biology, in which heâs planning to get a university degree.
About LIFE EXTENSION ADVOCACY FOUNDATION (LEAF)
In 2014, the Life Extension Advocacy Foundation was established as a 501(c)(3) non-profit organization dedicated to promoting increased healthy human lifespan through fiscally sponsoring longevity research projects and raising awareness regarding the societal benefits of life extension. In 2015 they launched Lifespan.io, the first nonprofit crowdfunding platform focused on the biomedical research of aging.
They believe that this will enable the general public to influence the pace of research directly. To date they have successfully supported four research projects aimed at investigating different processes of aging and developing therapies to treat age-related diseases.
The LEAF team organizes educational events, takes part in different public and scientific conferences, and actively engages with the public on social media in order to help disseminate this crucial information. They initiate public dialogue aimed at regulatory improvement in the fields related to rejuvenation biotechnology.