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August Weismann's 1892 germ plasm theory. The hereditary material, the germ plasm, is transmitted only by the gonads. Somatic cells (of the body) develop afresh in each generation from the germ plasm.
August Weismann proposed the germ plasm theory in the 19th century, before the foundation of modern genetics.

Germ plasm (German: Keimplasma) is a biological concept developed in the 19th century by the German biologist August Weismann. It states that heritable information is transmitted only by germ cells in the gonads (ovaries and testes), not by somatic cells. The related idea that information cannot pass from somatic cells to the germ line, contrary to Lamarckism, is called the Weismann barrier. To some extent this theory anticipated the development of modern genetics.

History

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The term Keimplasma (germ plasm) was first used by the German biologist, August Weismann (1834–1914), and described in his 1892 book Das Keimplasma: eine Theorie der Vererbung (The Germ Plasm: a theory of inheritance).[1] His theory states that multicellular organisms consist of germ cells that contain and transmit heritable information, and somatic cells which carry out ordinary bodily functions.[1][2] In the germ plasm theory, inheritance in a multicellular organism only takes place by means of the germ cells: the gametes, such as egg cells and sperm cells. Other cells of the body do not function as agents of heredity. The effect is one-way: germ cells produce somatic cells, and more germ cells; the germ cells are not affected by anything the somatic cells learn or any ability the body acquires during its life. Genetic information cannot pass from soma to germ plasm and on to the next generation. This is referred to as the Weismann barrier.[3] This idea, if true, rules out the inheritance of acquired characteristics as proposed by Jean-Baptiste Lamarck, like others before him, and accepted by Charles Darwin both in On the Origin of Species and as part of his pangenesis theory of inheritance.[4]

However, a careful reading of Weismann's work over the span of his entire career shows that he had more nuanced views. He insisted, like Darwin, that a variable environment was necessary to cause variation in the hereditary material.[2] Because genetic information cannot pass from soma to germ plasm, these external conditions, he believed, caused different effects on the soma and the germ plasm. Thus, the historian of science Rasmus G. Winther states, Weismann was not a Weismannian, as he, like Darwin, did believe in the inheritance of acquired characteristics, which later came to be known as Lamarckian.[2]

The part of Weismann's theory which proved most vulnerable was his notion that the germ plasm (effectively, genes) was successively reduced during division of somatic cells. As modern genetics developed, it became clear that this idea is wrong in most cases.[5] Cases such as Dolly, the cloned sheep, proved via somatic cell nuclear transfer that adult cells retain a complete set of information – as opposed to Weismann's increasingly determined gradual loss of genetic information – putting this aspect of Weismann's theory to rest as a general rule of metazoan development. However, genetic information is readily lost by somatic cells in some groups of animals through somatic genome processing. The best known example is the nematodes, in which the phenomenon of chromatin diminution was first described by Theodor Boveri in 1887.[6]

The idea was to some extent anticipated in an 1865 article by Francis Galton, published in Macmillan's Magazine, which set out a weak version of the concept. In 1889 Weismann wrote to acknowledge that "You have exposed in your paper an idea which is in one essential point nearly allied to the main idea contained in my theory of the continuity of germ-plasm".[7]

Modern view

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The idea of the Weismann barrier, namely that changes acquired during an organism's life cannot affect its offspring, is still broadly accepted. This has been extended into molecular terms as the central dogma of molecular biology, which asserts that information written in the form of proteins cannot be fed back into genetically transmissible information encoded in nucleic acids.[8]

The Weismannian notion that the germ cells are unaffected by somatic cells or their environment is however proving not to be absolute. Chemical modification of the nucleotide bases that constitute the genetic code such as methylation of cytosines as well as modifications of the histones around which DNA is organized into higher-order structures are influenced by the metabolic and physiologic state of the organism and in some cases can be heritable. Such changes are called epigenetic because they do not alter the nucleotide sequence.[9]

References

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Germ plasm

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Germ plasm is a foundational concept in biology denoting the specialized hereditary substance within germ cells—such as eggs and sperm—that transmits genetic information across generations, distinct from the somatoplasm of somatic (body) cells.[1] This idea, central to the germ plasm theory proposed by German biologist August Weismann in his 1893 book The Germ-Plasm: A Theory of Heredity, posits that heredity occurs exclusively through the continuous lineage of germ plasm, establishing a barrier (known as the Weismann barrier) that prevents acquired traits in somatic cells from influencing the germline.[1] Weismann's framework explained inheritance via a hierarchical structure of germinal units, including biophors (molecular particles), determinants (cell-specific groups), ids (nuclear structures), and idants (chromosomes), with amphimixis (fusion of gametes) enabling variation through reduction division and recombination.[1] In the historical context of late 19th-century biology, Weismann's theory emerged as a response to earlier ideas like Charles Darwin's pangenesis, which allowed for the inheritance of acquired characteristics, by emphasizing the immortality and isolation of germ plasm across generations.[1] It influenced the development of modern genetics by underscoring the separation of germline and soma, though it faced criticisms, such as from Hugo de Vries for overlooking intracellular mechanisms of variation.[1] Today, the term retains relevance in evolutionary biology as a metaphor for the continuity of genetic lineages, reinforcing principles like the central dogma of molecular biology that information flows unidirectionally from DNA to proteins without somatic feedback to the genome.[2] In contemporary developmental biology, germ plasm specifically refers to the asymmetrically localized cytoplasmic components in oocytes that direct the specification of primordial germ cells (PGCs) in many non-mammalian species, ensuring the formation of functional gametes.[3] These determinants typically include maternally inherited RNAs (e.g., nanos and Xpat), proteins, mitochondria, and germinal granules organized into polar aggregates, such as at the vegetal pole in Xenopus frogs or the posterior pole in Drosophila flies.[4] Unlike in mammals, where germline fate is induced zygotically via bone morphogenetic protein (BMP) signaling, germ plasm in species like nematodes, insects, fish, and amphibians provides a preformed, inheritance-based mechanism for germline determination, highlighting evolutionary diversity in reproductive cell lineage establishment.[5] This modern usage builds on Weismann's legacy while integrating molecular insights, such as the role of ribonucleoprotein particles in translational repression and cell fate commitment.[6]

Definition and Core Concepts

Definition

Germ plasm refers to the hereditary substance contained within germ cells, such as sperm and egg cells, that transmits genetic information unchanged from one generation to the next, separate from the non-reproductive somatic tissues of the body.[7] This material ensures the continuity of hereditary traits solely through reproductive lineages, preventing the inheritance of modifications acquired during an organism's lifetime.[1] As a theoretical construct, germ plasm represents the immortal chain of genetic determinants that persists across generations, forming the basis for understanding heredity in multicellular organisms.[1] Proposed in the late 19th century by August Weismann, it posits that this substance is sequestered early in development and safeguarded from somatic influences. The term has dual usage: in its historical sense, it denotes the continuous germline material; in modern developmental biology, it specifically refers to asymmetrically localized cytoplasmic determinants (such as RNAs and proteins) in oocytes of many non-mammalian species that specify primordial germ cells (PGCs).[7] In animals, germ plasm is localized within primordial germ cells during embryogenesis, where it directs the formation of gametes and maintains the germline's integrity.[8]

Germ Plasm vs. Soma

In Weismann's germ plasm theory, the soma refers to the non-reproductive cells of the body that perform essential functions during an organism's lifetime but are considered disposable and incapable of transmitting acquired modifications to offspring.[1] These somatic cells, such as those forming skin, muscles, or organs, can undergo changes due to environmental influences, injury, or aging, yet such alterations remain confined to the individual and do not affect the hereditary lineage.[9] This distinction underscores a fundamental separation between the germ plasm and soma: the germ plasm, housed within reproductive germ cells, remains continuous across generations and is insulated from somatic influences, thereby ensuring the stability of inherited traits.[1] In contrast, the soma supports the organism's survival and reproduction—providing nourishment and protection to germ cells—but is not immortal, as it deteriorates over time without contributing to heredity.[10] This insulation, often termed the Weismann barrier, prevents environmental impacts on the body from altering the genetic material passed to descendants, promoting evolutionary change solely through selection on germinal variations.[9] A useful analogy portrays the germ plasm as a protected archive safeguarding hereditary information, while the soma functions as the working machinery of daily life, subject to wear but unable to rewrite the archive.[1] In multicellular organisms like humans, this is exemplified by germ cells sequestered in the gonads (such as oocytes and spermatogonia), which remain isolated from the broader somatic tissues like epidermal skin cells or cardiac muscle fibers that interact directly with the environment.[10] This oppositional relationship is central to the theory, as it rejects the inheritance of traits acquired by the soma during an organism's life.[9]

Historical Development

Precursors to the Theory

In the 17th and 18th centuries, preformationism emerged as a dominant theory of generation and heredity, positing that organisms develop from miniature, fully formed versions of themselves already present in the gametes. Proponents, known as spermists, argued that tiny homunculi—complete miniature adults—resided within sperm cells, as illustrated by Antonie van Leeuwenhoek's microscopic observations of spermatozoa in 1677 and Nicolaas Hartsoeker's 1694 depiction of a folded human figure in the sperm head.[11] In contrast, ovists maintained that preformed organisms existed in the egg, a view supported by early embryological studies of chick development by Marcello Malpighi in the 1670s.[11] This theory implied a continuous chain of preformed generations encapsulated within one another, extending back to the biblical creation, and framed heredity as the mechanical unfolding of these preexisting structures rather than the emergence of new forms.[12] By the late 18th century, preformationism began evolving amid challenges from epigenesis advocates like Caspar Friedrich Wolff, who in 1759 described development as a gradual process of part formation from unorganized material.[12] This shift influenced emerging ideas of hereditary particles, with figures such as Pierre-Louis Moreau de Maupertuis proposing in 1745 that invisible organic molecules from parents combined to produce offspring traits, blending elements of both theories.[11] Similarly, Georges-Louis Leclerc, Comte de Buffon, introduced in his 1749 Histoire Naturelle the concept of moldable organic molecules sensitive to environmental influences, laying groundwork for particulate views of inheritance that moved beyond rigid preformation toward dynamic hereditary units.[11] A significant precursor came from Charles Darwin's provisional hypothesis of pangenesis, outlined in 1868, which suggested that all body parts contribute to heredity through gemmules—tiny, modifiable particles shed by cells and circulated throughout the organism before concentrating in the reproductive cells.[13] These gemmules, capable of remaining dormant across generations or being altered by use and environment, explained phenomena like reversion to ancestral traits and the potential inheritance of acquired characteristics, such as strengthened organs in domesticated animals.[13] Darwin's model unified heredity with development and variation, portraying the body as a collective contributor to the germline, though it implied a permeable boundary between somatic and reproductive elements. Building on such ideas, Carl Nägeli advanced a more structured distinction in 1884 by differentiating idioplasm, the organized hereditary substance composed of arranged micellae carrying developmental determinants, from trophoplasm, the watery nutritive plasma responsible for cellular nutrition and growth but not inheritance.[14] In Nägeli's view, idioplasm formed a continuous, evolving framework within cells that transmitted traits across generations via germ cells, while trophoplasm supported individual ontogeny without influencing phylogeny, thus isolating heredity from somatic changes.[14] This separation prefigured later theories by emphasizing a specialized hereditary material immune to bodily influences.

Weismann's Formulation

August Weismann formalized his germ plasm theory in the 1893 publication The Germ-Plasm: A Theory of Heredity, where he synthesized earlier ideas into a comprehensive framework for understanding heredity.[1] This work built upon his prior experiments from the 1880s, notably the tail-cutting studies on mice conducted between 1882 and 1888, in which he removed the tails of 68 mice over five generations, which produced 901 offspring, to test for the inheritance of acquired characteristics.[15] The results showed no reduction in tail length among offspring, providing empirical evidence against Lamarckian inheritance and supporting the notion that modifications to somatic tissues do not affect hereditary material.[15] In his formulation, Weismann proposed that heredity occurs exclusively through the germ plasm, a specialized hereditary substance contained within germ cells and isolated from the somatoplasm of body cells.[1] He conceptualized the germ plasm as a complex structure composed of idioplasms—molecular units organized hierarchically into biophors (the smallest vital units), determinants (groups controlling organ formation), ids (clusters directing cell types), and idants (chromosome-level aggregates).[1] These idioplasms remain unchanged across generations, ensuring the continuity of hereditary information while preventing any influence from somatic changes, thus establishing a unidirectional flow from germ plasm to soma.[1] A key experimental basis for this separation was Weismann's integration of cytological observations on chromosome behavior during germ cell division, drawing from contemporary findings such as Theodor Boveri and Eduard Strasburger's 1888 demonstrations of reduction division in sex cells.[1] These showed that germ cells contain half the number of chromosomes (idants) found in somatic cells, providing a physical mechanism for the isolation and continuity of the germ plasm without dilution during development.[1] Weismann argued that the germ plasm must consist of an immense number of such particles to accommodate the progressive reduction through countless cell divisions in multicellular organisms, allowing for precise distribution to diverse cell lineages.[16]

Key Principles and Mechanisms

Continuity of Germ Plasm

The principle of continuity posits that germ plasm, the hereditary substance residing in germ cells, is transmitted unchanged from parent to offspring exclusively through gametes, forming a perpetual lineage that spans generations. This transmission ensures that the germ plasm remains identical in composition across successive individuals, independent of any alterations arising in somatic tissues during an organism's lifetime. Weismann articulated this as the foundational basis of heredity, emphasizing that the germ plasm constitutes a stable, self-perpetuating entity that links all members of a species in an unbroken sequence. During embryogenesis, the continuity is mechanistically upheld through the early segregation of germ plasm into primordial germ cells, which are set aside from the outset of development to safeguard the hereditary material from somatic influences. In multicellular organisms, this segregation occurs shortly after fertilization, directing a portion of the zygotic germ plasm toward the formation of the germ line while the remainder contributes to somatic lineages. This process, as described by Weismann, maintains the purity of the germ plasm by isolating it from the differentiating body cells, thereby preventing any dilution or modification through environmental or physiological changes in the soma. Theoretically, this uninterrupted continuity underpins the stability and constancy of species characteristics over time, as variations in the germ plasm alone can propagate to future generations. A critical aspect preserving this integrity is the reduction division in meiosis, which Weismann identified as halving the quantity of germ plasm in each gamete to counteract the doubling that would otherwise occur with ordinary cell divisions. For example, in observations of chromosomal behavior during gamete formation, this reductive mechanism ensures that the hereditary determinants do not accumulate excessively, thereby sustaining the balanced transmission essential for species persistence.

The Weismann Barrier

The Weismann barrier refers to the proposed impermeable separation between the germ line and the somatic cells within an organism, ensuring that changes or influences arising in the soma—such as acquired traits from environmental adaptations or injuries—cannot feedback into the hereditary material carried by germ cells. This concept, central to August Weismann's germ plasm theory, posits that the germ plasm, as the continuous hereditary substance, remains isolated from somatic modifications, thereby preserving the integrity of genetic transmission across generations. Weismann's formulation of the barrier's basis drew from cytological observations of early embryonic development, where he argued that germ plasm determinants are sequestered and shielded within specific gonadal precursor cells from the outset, preventing any mingling with somatic cell lineages. In his 1893 work The Germ-Plasm: A Theory of Heredity, he described this separation as occurring through a hierarchical organization of hereditary units—ranging from biophors to ids and idants—confined to the nuclear material of germ cells, which are set aside early and remain unaffected by the body's physiological processes. This cytological divide was intended to explain why somatic development, while derived from the germ plasm, does not reciprocally alter it, maintaining a unidirectional flow of hereditary information. A key consequence of the Weismann barrier is its prediction that mutilations or adaptive changes to the soma will not be inherited by offspring, as these alterations do not reach the protected germ plasm. To test this, Weismann conducted an experiment in which he removed the tails of 68 white mice over five generations, reporting that 901 offspring were produced, all with tails of normal length.[17] This outcome underscored the barrier's function as a protective mechanism, aligning with the broader principle of germ plasm continuity by isolating hereditary material from non-genetic influences.

Implications and Criticisms

Rejection of Lamarckian Inheritance

Jean-Baptiste Lamarck proposed in his 1809 work Philosophie zoologique that organisms could inherit traits acquired during their lifetime through the use or disuse of organs, driven by environmental needs and habits.[18] This theory, known as Lamarckism or the inheritance of acquired characteristics, posited that such changes were heritable and accumulated over generations to drive evolutionary adaptation.[19] A classic example is Lamarck's explanation for the long neck of the giraffe, where ancestral giraffes allegedly stretched to reach higher foliage in resource-scarce environments, gradually lengthening their necks through repeated use, with this trait passed to offspring.[18] August Weismann's germ plasm theory directly refuted this idea by establishing a strict separation between the soma (body cells) and the germ plasm (hereditary material in germ cells).[1] In his 1893 book The Germ-Plasm: A Theory of Heredity, Weismann argued that somatic adaptations, such as increased muscle mass from exercise or injury-induced changes, occur only in non-reproductive cells and cannot influence the immutable germ plasm, which remains isolated by the Weismann barrier.[1] Weismann supported this rejection through experiments demonstrating the non-inheritance of somatic alterations. In one notable experiment, he cut off the tails of mice over multiple generations—initially 5 generations involving 901 mice, later extended to 22 generations—and observed no shortening in the tails of offspring, illustrating that such somatic modifications are not heritable.[20] Thus, acquired characteristics represent "soft inheritance" that fails to transmit across generations, as the germ plasm's continuity ensures heredity derives solely from pre-existing determinants rather than environmental modifications to the body.[20] This theoretical opposition had profound implications for evolutionary biology, redirecting focus from Lamarckian use-inheritance to Darwinian natural selection acting on heritable variations originating in the germ plasm.[20] By emphasizing mutations or recombinations within the germ line as the source of variation, Weismann's framework reinforced the primacy of selection on fixed genetic material, paving the way for modern genetics and diminishing the role of acquired traits in long-term adaptation.[1]

Early Criticisms and Experimental Challenges

One of the earliest significant critiques of Weismann's germ plasm theory came from geneticist Thomas Hunt Morgan in the 1910s, who used experiments on the fruit fly Drosophila melanogaster to challenge the theory's conceptualization of the germ plasm as a complex, hierarchical structure of "idioplasm" composed of numerous specialized particles or determinants. Morgan's discovery of sex-linked inheritance in 1910, followed by observations of gene linkage and crossing over in 1911–1915, demonstrated that hereditary factors were linearly arranged on chromosomes, suggesting a simpler, more particulate basis for the germ plasm than Weismann's elaborate model of idioplasm with branching developmental pathways. These findings implied that the germ plasm's variability arose through chromosomal recombination and mutations rather than the intricate rearrangements Weismann proposed, rendering the idioplasm's complexity unnecessary and speculative.[21][22][2] Experimental efforts to test the theory's core tenet of an absolute Weismann barrier—isolating the germ plasm from somatic influences—revealed partial successes in inducing heritable changes, thereby questioning its rigidity. Botanist Hugo de Vries's mutation theory, introduced in 1901 based on observations of sudden, large-scale variations in Oenothera lamarckiana, posited that the germ plasm could undergo abrupt, internal saltatory changes independent of gradual selection, introducing variability directly into the hereditary material and challenging Weismann's emphasis on continuous, incremental modifications through amphimixis alone.[1] Later, in 1927, geneticist Hermann Joseph Muller demonstrated that X-ray irradiation of Drosophila germ cells induced heritable mutations at rates far exceeding spontaneous ones—up to 150 times higher for lethal mutations—showing that external physical agents could directly alter the germ plasm, thus piercing the barrier's supposed impermeability to environmental impacts on heredity. These results highlighted the germ plasm's susceptibility to induced variability, undermining the theory's claim of complete isolation.[23] Internally, Weismann's framework faced criticism for its arbitrary assumptions, particularly regarding the structure and number of particles in the idioplasm, which lacked empirical grounding and led to broader debates on inheritance mechanisms. Weismann posited that the idioplasm consisted of a fixed, hierarchical array of micronuclear and macronuclear determinants—initially assuming a progressive reduction in their number across somatic cell divisions to explain development—but this quantification was deemed ad hoc, as it failed to align with observed cellular divisions and required constant revisions without supporting evidence. The theory's absence of molecular-level detail further fueled disputes between blending inheritance advocates, who saw traits as averaging across generations, and particulate proponents like Morgan, who argued for discrete, stable units; Weismann's model, while particulate in intent, offered no mechanism to resolve how such particles avoided blending during reproduction, exposing foundational gaps.[24]

Modern Interpretations

Integration with Molecular Genetics

In the framework of molecular genetics, Weismann's germ plasm has been reinterpreted as the genomic DNA sequestered within germ cells, serving as the immutable carrier of hereditary information across generations.[25] This alignment posits the germ plasm's continuity through precise DNA replication during mitotic divisions in the germline and equitable distribution via meiotic segregation, ensuring stable transmission of genetic determinants while generating variation through recombination and mutation.[25] The Weismann barrier, originally conceived as an impenetrable divide between germinal and somatic lineages, corresponds to the developmental sequestration of primordial germ cells early in embryogenesis, isolating the germline from somatic influences and preserving the integrity of heritable material.[25] Key experimental milestones in the mid-20th century substantiated this molecular equivalence. The 1944 Avery-MacLeod-McCarty experiment demonstrated that DNA, rather than protein, functions as the transforming principle capable of inducing heritable changes in bacterial traits, thereby identifying it as the fundamental hereditary substance long anticipated by germ plasm theory. Complementing this, the 1953 Watson-Crick model elucidated DNA's double-helical structure, with complementary base pairing enabling semi-conservative replication that faithfully propagates genetic information—a mechanism that mechanistically fulfills Weismann's vision of an indestructible, continuous germ plasm. Contemporary genomic analyses further validate these principles, revealing that germline mutations, arising during DNA replication in germ cells, constitute the primary source of heritable variation driving evolutionary change, as predicted by Weismann's emphasis on germline-exclusive inheritance. Whole-genome sequencing of parent-offspring trios has quantified de novo germline mutation rates at approximately 1-2 × 10^{-8} per nucleotide per generation in humans, underscoring how such events, isolated from somatic alterations by the Weismann barrier, fuel adaptive evolution without Lamarckian reversion.[26] This molecular synthesis thus refines the classical theory, portraying germ plasm not as an abstract vital force but as the dynamic, DNA-based archive of lineage continuity.[25]

Influence of Epigenetics

Epigenetics encompasses heritable modifications to gene expression that occur without changes to the DNA sequence, including mechanisms such as DNA methylation, histone modifications, and non-coding RNA activity. These processes can enable the transmission of environmental influences across generations via the germline, thereby modifying the traditional view of the germ plasm as an impermeable carrier of hereditary information.[27] In the nematode Caenorhabditis elegans, transgenerational epigenetic inheritance operates primarily through RNA-mediated pathways, where small RNAs respond to environmental cues and persist in the germline. For example, exposure to the pathogenic bacterium Pseudomonas aeruginosa PA14 triggers the production of P11 small RNAs, which are necessary and sufficient for transmitting pathogen avoidance behavior across four generations (P0 to F4), with inheritance dependent on temperature and medium conditions.[28] Histone modifications, such as H3K9 and H3K36 methylation, along with Argonaute proteins like NRDE-3 and HRDE-1, further facilitate the heritable cellular changes associated with associative learning, such as odor avoidance linked to starvation, transmitted via sperm to F1 and F2 descendants.[29] Evidence from mammalian studies, including the Dutch Hunger Winter famine (1944–1945), demonstrates persistent epigenetic alterations in exposed individuals and their descendants. Prenatal undernutrition during this period leads to reduced DNA methylation at the insulin-like growth factor 2 (IGF2) differentially methylated region, correlating with increased risks of metabolic and cardiovascular disorders in adulthood, with cohort analyses extending into the 2020s revealing intergenerational patterns in stress-related gene expression.[30][31] These observations indicate that famine-induced epigenetic marks can influence offspring health beyond direct exposure, though true transgenerational effects (F3 and beyond) remain debated in humans.[32] Such epigenetic mechanisms imply a nuanced revision to the germ plasm model, where the continuity of genetic material is preserved, but superimposed marks allow limited somatic or environmental inputs to affect heredity without breaching the fundamental DNA framework. This softens the rigidity of the Weismann barrier, as epigenetic information integrates into the germ plasm, though its stability remains under investigation through techniques like CRISPR-based epigenome editing, which reveal dynamic reprogramming in the germline.[27] Recent studies confirm that while mutations can enhance mark persistence, environmental transmission in vertebrates is often constrained, maintaining the core isolation of germ line heredity.[33]

References

  1. The Germ-Plasm: a Theory of Heredity (1893), by August Weismann
  2. [PDF] August Weismann on Germ-Plasm Variation
  3. Germplasm - an overview | ScienceDirect Topics
  4. https://www.sciencedirect.com/science/article/pii/S0070215315000575
  5. https://www.sciencedirect.com/science/article/pii/B9780123849519000071
  6. https://www.sciencedirect.com/science/article/pii/S0070215319301073
  7. Modeling germ cell differentiation - StemBook - NCBI Bookshelf
  8. Environmentally Induced Epigenetic Transgenerational Inheritance ...
  9. Primordial Germ Cell Specification and Migration - PMC - NIH
  10. The Distinction Between Innate and Acquired Characteristics (Stanford Encyclopedia of Philosophy)
  11. The deteriorating soma and the indispensable germline: gamete ...
  12. Chip Off the Old Block: Generation, Development, and Ancestral ...
  13. Theories of Biological Development (Stanford Encyclopedia of Philosophy)
  14. Darwin, C. R. 1868. The variation of animals and plants under ...
  15. A Mechanico-Physiological Theory of Organic Evolution
  16. August Friedrich Leopold Weismann (1834-1914)
  17. ESP Digital Books: The Germ-Plasm: A Theory of Heredity
  18. What Is Lost in the Weismann Barrier? - PMC - NIH
  19. Lamarck, Evolution, and the Inheritance of Acquired Characters - PMC
  20. Zoological philosophy; : Lamarck, Jean Baptiste Pierre Antoine de ...
  21. “Sex Limited Inheritance in Drosophila” (1910), by Thomas Hunt ...
  22. [PDF] The Theory of the Gene. - ESP.ORG
  23. Hermann Joseph Muller's Study of X-rays as a Mutagen, (1926-1927)
  24. A Critique of the Theory of Evolution. - Project Gutenberg
  25. https://doi.org/10.3390/jdb8040035
  26. Transgenerational epigenetic inheritance: a critical perspective
  27. Molecular requirements for C. elegans transgenerational epigenetic ...
  28. Inheritance of associative memories and acquired cellular changes ...
  29. Epigenetics and transgenerational inheritance - Moelling - 2024
  30. A critical view on transgenerational epigenetic inheritance in humans
  31. https://doi.org/10.1016/j.cell.2022.12.047
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