Maximum life span


Maximum life span is a measure of the maximum amount of time one or more members of a population have been observed to survive between birth and death. The term can also denote an estimate of the maximum amount of time that a member of a given species could survive between birth and death, provided circumstances that are optimal to that member's longevity.
Most living species have at least one upper limit on the number of times the cells of a member can divide. This is called the Hayflick limit, although number of cell divisions does not strictly control lifespan.

Definition

In animal studies, maximum span is often taken to be the mean life span of the most long-lived 10% of a given cohort. By another definition, however, maximum life span corresponds to the age at which the oldest known member of a species or experimental group has died. Calculation of the maximum life span in the latter sense depends upon initial sample size.
Maximum life span contrasts with mean life span , and longevity. Mean life span varies with susceptibility to disease, accident, suicide and homicide, whereas maximum life span is determined by "rate of aging". Longevity refers only to the characteristics of the especially long lived members of a population, such as infirmities as they age or compression of morbidity, and not the specific life span of an individual.
If age x is subtracted from the hypothetical upper limit w for the species and logs are taken, then the resulting variable log is normally distributed similarly as all natural quantitative variables resulting from gene expression. This is due to the law of large numbers, the Central Limit Theorem.

In humans

The longest living person whose dates of birth and death were verified according to the modern norms of Guinness World Records and the Gerontology Research Group was Jeanne Calment, a French woman who reportedly lived to 122. Reduction of infant mortality has accounted for most of the increased average life span longevity, but since the 1960s mortality rates among those over 80 years have decreased by about 1.5% per year. "The progress being made in lengthening lifespans and postponing senescence is entirely due to medical and public-health efforts, rising standards of living, better education, healthier nutrition and more salubrious lifestyles." Animal studies suggest that further lengthening of median human lifespan as well as maximum lifespan could be achieved through "calorie restriction mimetic" drugs or by directly reducing food consumption. Although calorie restriction has not been proven to extend the maximum human life span, as of 2014, results in ongoing primate studies have demonstrated that the assumptions derived from rodents are valid in primates as well .
It has been proposed that no fixed theoretical limit to human longevity is apparent today. Studies in the biodemography of human longevity indicate a late-life mortality deceleration law: that death rates level off at advanced ages to a late-life mortality plateau. That is, there is no fixed upper limit to human longevity, or fixed maximal human lifespan. This law was first quantified in 1939, when researchers found that the one-year probability of death at advanced age asymptotically approaches a limit of 44% for women and 54% for men.
However, this evidence depends on the existence of a late-life plateaus and deceleration that can be explained, in humans and other species, by the existence of very rare errors. Age-coding error rates below 1 in 10,000 are sufficient to make artificial late-life plateaus, and errors below 1 in 100,000 can generate late-life mortality deceleration. These error rates cannot be ruled out by examining documents, the standard because successful pension fraud, identity theft, forgeries and errors that leave no documentary evidence. This capacity for errors to explain late-life plateaus solves the "fundamental question in aging research is whether humans and other species possess an immutable life-span limit.", indicating that humans do indeed have a lifespan limit.
Scientists have observed that a person's VO2max value decreases as a function of age. Therefore, the maximum lifespan of a person could be determined by calculating when the person's VO2max value drops below the basal metabolic rate necessary to sustain life, which is approximately 3 ml per kg per minute. On the basis of this hypothesis, athletes with a VO2max value between 50 and 60 at age 20 would be expected "to live for 100 to 125 years, provided they maintained their physical activity so that their rate of decline in VO2max remained constant".
Longitudinal variations of physiological indices, such as complete blood counts, along individual aging trajectories revealed a linear increase of the organism state fluctuations range with age. The broadening could be explained by a progressive loss of physiological resilience measured by the individual blood factors inverse auto-correlation times. Extrapolation of this data suggested that organism state recovery time and variance would simultaneously diverge at a critical point of 120 – 150 years of age corresponding to a complete loss of resilience and hence should be incompatible with survival. The criticality resulting in the end of life is an intrinsic biological property of an organism that is independent of stress factors and signifies a fundamental or absolute limit of human lifespan.
A theoretical study suggested the maximum human lifespan to be around 125 years using a modified stretched exponential function for human survival curves. The analysis of dynamics of the body mass in human population indicates extremums, which correspond to mean, the commonly accepted maximum and maximum known lifespan.
In another study, researchers claimed that there exists a maximum lifespan for humans, and that the human maximal lifespan has been declining since the 1990s.
This study is now disputed on the basis of simple coding errors and biased sampling. This study also supports a continuing increase in both theoretical and observed upper human lifespan, based on observed data from 200 national populations. However, a theoretical study also suggested that the maximum human life expectancy at birth is limited by the human life characteristic value δ, which is around 104 years.
The United Nations has undertaken an important . The 2017 95% prediction interval of 2090 average life expectancy rises as high as +6 by 2090, with dramatic, ongoing, layered consequences on world population and demography should that happen. The prediction interval is extremely wide, and the United Nations can not be certain. Organizations like the Methuselah Foundation are working toward an end to senescence and practically unlimited human lifespan. If successful, the demographic implications for human population will be greater in effective multiplier terms than any experienced in the last five centuries if maximum lifespan or the birthrate remain unlimited by law. Modern Malthusian predictions of overpopulation based on increased longevity have been criticized on the same basis as general population alarmism.

In other animals

Small animals such as birds and squirrels rarely live to their maximum life span, usually dying of accidents, disease or predation.
The maximum life span of most species is documented in the Anage repository.
Maximum life span is usually longer for species that are larger or have effective defenses against predation, such as bird flight, chemical defenses or living in social groups.
The differences in life span between species demonstrate the role of genetics in determining maximum life span. The records are these:
The longest-lived vertebrates have been variously described as
Invertebrate species which continue to grow as long as they live can on occasion live hundreds of years:
s are referred to as annuals which live only one year, biennials which live two years, and perennials which live longer than that. The longest-lived perennials, woody-stemmed plants such as trees and bushes, often live for hundreds and even thousands of years. A giant sequoia, General Sherman is alive and well in its third millennium. A Great Basin Bristlecone Pine called Methuselah is 4,848 years old and the Bristlecone Pine called Prometheus was a little older still, at least 4,844 years, when it was cut down in 1964. The oldest known plant is a clonal Quaking Aspen tree colony in the Fishlake National Forest in Utah called Pando at about 80,000 years. Lichen, a symbiotic algae and fungal proto-plant, such as Rhizocarpon geographicum can live upwards of 10,000 years.

Increasing maximum life span

"Maximum life span" here means the mean life span of the most long-lived 10% of a given cohort. Caloric restriction has not yet been shown to break mammalian world records for longevity. Rats, mice, and hamsters experience maximum life-span extension from a diet that contains all of the nutrients but only 40–60% of the calories that the animals consume when they can eat as much as they want. Mean life span is increased 65% and maximum life span is increased 50%, when caloric restriction is begun just before puberty. For fruit flies the life extending benefits of calorie restriction are gained immediately at any age upon beginning calorie restriction and ended immediately at any age upon resuming full feeding.
A few transgenic strains of mice have been created that have maximum life spans greater than that of wild-type or laboratory mice. The Ames and Snell mice, which have mutations in pituitary transcription factors and hence are deficient in Gh, LH, TSH, and secondarily IGF1, have extensions in maximal lifespan of up to 65%. To date, both in absolute and relative terms, these Ames and Snell mice have the maximum lifespan of any mouse not on caloric restriction. Mutations/knockout of other genes affecting the GH/IGF1 axis, such as Lit, Ghr and Irs1 have also shown extension in lifespan, but much more modest both in relative and absolute terms. The longest lived laboratory mouse ever was a Ghr knockout mouse, which lived to ≈1800 days in the lab of Andrzej Bartke at Southern Illinois University. The maximum for normal B6 mice under ideal conditions is 1200 days.
Most biomedical gerontologists believe that biomedical molecular engineering will eventually extend maximum lifespan and even bring about rejuvenation.Anti-aging drugs are a potential tool for extending life.
Aubrey de Grey, a theoretical gerontologist, has proposed that aging can be reversed by Strategies for Engineered Negligible Senescence. De Grey has established The Methuselah Mouse Prize to award money to researchers who can extend the maximum life span of mice. So far, three Mouse Prizes have been awarded: one for breaking longevity records to Dr. Andrzej Bartke of Southern Illinois University ; one for late-onset rejuvenation strategies to Dr. Stephen Spindler of the University of California ; and one to Dr. Z. Dave Sharp for his work with the pharmaceutical rapamycin.

Correlation with DNA repair capacity

Accumulated DNA damage appears to be a limiting factor in the determination of maximum life span. The theory that DNA damage is the primary cause of aging, and thus a principal determinant of maximum life span, has attracted increased interest in recent years. This is based, in part, on evidence in human and mouse that inherited deficiencies in DNA repair genes often cause accelerated aging. There is also substantial evidence that DNA damage accumulates with age in mammalian tissues, such as those of the brain, muscle, liver and kidney. One expectation of the theory is that among species with differing maximum life spans, the capacity to repair DNA damage should correlate with lifespan. The first experimental test of this idea was by Hart and Setlow who measured the capacity of cells from seven different mammalian species to carry out DNA repair. They found that nucleotide excision repair capability increased systematically with species longevity. This correlation was striking and stimulated a series of 11 additional experiments in different laboratories over succeeding years on the relationship of nucleotide excision repair and life span in mammalian species. In general, the findings of these studies indicated a good correlation between nucleotide excision repair capacity and life span. The association between nucleotide excision repair capability and longevity is strengthened by the evidence that defects in nucleotide excision repair proteins in humans and rodents cause features of premature aging, as reviewed by Diderich.
Further support for the theory that DNA damage is the primary cause of aging comes from study of Poly ADP ribose polymerases. PARPs are enzymes that are activated by DNA strand breaks and play a role in DNA base excision repair. Burkle et al. reviewed evidence that PARPs, and especially PARP-1, are involved in maintaining mammalian longevity. The life span of 13 mammalian species correlated with polyation capability measured in mononuclear cells. Furthermore, lymphoblastoid cell lines from peripheral blood lymphocytes of humans over age 100 had a significantly higher polyation capability than control cell lines from younger individuals.

Research data