scholarly journals THE MECHANISM OF ACCUMULATION IN LIVING CELLS

1952 ◽  
Vol 35 (4) ◽  
pp. 579-594 ◽  
Author(s):  
W. J. V. Osterhout
Keyword(s):  
Osmotic Pressure ◽  
Outer Surface ◽  
Organic Molecules ◽  
Sea Water ◽  
Relative Rate ◽  
Point Of View ◽  
External Concentration ◽  
Protoplasmic Surface ◽  
A Cell ◽  
Outer Protoplasmic Surface

When a compound enters a living cell until its activity becomes greater inside than outside, it may be said to accumulate. Since it moves from a region where its activity is relatively low to a region where its activity is relatively high, it is evident that work must be done to bring this about. The following explanation is suggested to account for accumulation. The protoplasmic surface is covered with a non-aqueous layer which is permeable to molecules but almost impermeable to ions. Hence free ions cannot enter except in very small numbers. The experiments indicate that ions combine at the outer surface with organic molecules (carrier molecules) and are thus able to enter freely. If upon reaching the aqueous protoplasm these molecules are decomposed or altered so as to set the ions free, the ions must be trapped since they cannot pass out except in very small numbers. If we adopt this point of view we can suggest answers to some important questions. Among these are the following: 1. Why accumulation is confined to electrolytes. This is evident since only ions will be trapped. 2. Why ions appear to penetrate against a gradient. Actually there is no such penetration since the ions enter in combination with molecules. The energy needed to raise the activity of entering compounds is furnished by the reactions involved in the process of accumulation. 3. Why, in absence of injury, ions do not come out when the cell is placed in distilled water. Presumably the outgoing ions will combine at the outer surface with carrier molecules and then move inward in the same way as ions coming from without. 4. Why the relative rate of penetration falls off as the external concentration increases. This is because the entrance of ions is limited by the number of carrier molecules but no such limitation exists when ions move outward since they can do so without combining with carrier molecules. 5. Why accumulation is promoted by constructive metabolism which is needed to build up the organic molecules and by destructive metabolism which brings about their decomposition. 6. Why measuring the mobilities of ions in the outer protoplasmic surface does not enable us to predict the relative rate of entrance of ions. We find for example in Nitella that K+ has a much higher mobility than Na+ but the accumulation of these ions does not differ greatly. This is to be expected if they enter by combining with molecules at the surface. Only if K+ is able to combine preferentially will it accumulate preferentially. 7. Why ions may come out in anoxia and at low temperatures. If these conditions depress the formation of carrier molecules and their decomposition in the protoplasm, the balance between intake and outgo of ions will be disturbed and relatively more may come out. 8. Why the excess of internal over external osmotic pressure is less in sea water than in fresh water. As the external concentration of ions increases the rate of intake does not increase in direct proportion since the number of carrier molecules does not increase and this slows down the relative rate of intake of ions. But it does not slow down the rate of exit of ions since they need not combine with carrier molecules in order to pass out. Hence the excess of ions inside will be relatively less as the concentration of external ions increases. 9. How water is pumped from solutions of higher to solutions of lower osmotic pressure. If metabolism and consequently accumulation is higher at one end of a cell than at the other, the internal osmotic pressure will be higher at the more active end and this makes it possible for the cell to pump water from solutions of higher osmotic pressure at the more active end to solutions of lower osmotic pressure at the less active, as shown experimentally for Nitella. This might help to explain the action of kidney cells and the production of root pressure in plants.

scholarly journals THE KINETICS OF PENETRATION

1937 ◽  
Vol 20 (5) ◽  
pp. 737-766 ◽  
Author(s):  
A. G. Jacques
Keyword(s):  
Sea Water ◽  
Surface Layers ◽  
Marked Contrast ◽  
External Concentration ◽  
Protoplasmic Surface ◽  
Kinetics Of ◽  
External Ph

When 0.1 M NaI is added to the sea water surrounding Valonia iodide appears in the sap, presumably entering as NaI, KI, and HI. As the rate of entrance is not affected by changes in the external pH we conclude that the rate of entrance of HI is negligible in comparison with that of NaI, whose concentration is about 107 times that of HI (the entrance of KI may be neglected for reasons stated). This is in marked contrast with the behavior of sulfide which enters chiefly as H2S. It would seem that permeability to H2S is enormously greater than to Na2S. Similar considerations apply to CO2. In this respect the situation differs greatly from that found with iodide. NaI enters because its activity is greater outside than inside so that no energy need be supplied by the cell. The rate of entrance (i.e. the amount of iodide entering the sap in a given time) is proportional to the external concentration of iodide, or to the external product [N+]o [I-lo, after a certain external concentration of iodide has been reached. At lower concentrations the rate is relatively rapid. The reasons for this are discussed. The rate of passage of NaI through protoplasm is about a million times slower than through water. As the protoplasm is mostly water we may suppose that the delay is due chiefly to the non-aqueous protoplasmic surface layers. It would seem that these must be more than one molecule thick to bring this about. There is no great difference between the rate of entrance in the dark and in the light.

scholarly journals ACTION CURVES WITH SINGLE PEAKS IN NITELLA IN RELATION TO THE MOVEMENT OF POTASSIUM

1940 ◽  
Vol 23 (6) ◽  
pp. 743-748 ◽  
Author(s):  
W. J. V. Osterhout ◽  
S. E. Hill
Keyword(s):  
Outer Surface ◽  
Distilled Water ◽  
Protoplasmic Surface ◽  
Outer Protoplasmic Surface ◽  
Two Peaks

In Nitella the action curve has two peaks, apparently because both protoplasmic surfaces (inner and outer) are sensitive to K+. Leaching in distilled water makes the outer surface insensitive to K+. We may therefore expect the action curve to have only one peak. This expectation is realized. The action curve thus obtained resembles that of Chara which has an outer protoplasmic surface that is normally insensitive to K+. The facts indicate that the movement of K+ plays an important part in determining the shape of the action curve.

scholarly journals STUDIES OF THE INNER AND OUTER PROTOPLASMIC SURFACES OF LARGE PLANT CELLS

1943 ◽  
Vol 27 (2) ◽  
pp. 139-142 ◽  
Author(s):  
W. J. V. Osterhout
Keyword(s):  
Osmotic Pressure ◽  
Outer Surface ◽  
Plant Cells ◽  
Central Vacuole ◽  
Electrical Measurements ◽  
Surface Layers ◽  
Large Plant ◽  
Protoplasmic Surface

In Nitella, Chara, Hydrodictyon, and Valonia the inner and outer non-aqueous protoplasmic surface layers can be separated by certain plasmolytic agents which penetrate the outer surface more rapidly than the inner and hence raise the osmotic pressure of the protoplasm lying between them and cause it to increase in thickness by taking up water from the central vacuole. We may therefore conclude that the two surfaces differ. This idea is confirmed by earlier electrical measurements which show that when sap is placed outside the cell the chain See PDF for Structure produces an E.M.F. of several millivolts.

scholarly journals A New Type of Luminescence in Fishes. II.

1926 ◽  
Vol 14 (2) ◽  
pp. 495-507 ◽  
Author(s):  
C. F. Hickling
Keyword(s):  
Osmotic Pressure ◽  
Sea Water ◽  
Adverse Conditions ◽  
Hypertonic Solutions ◽  
Typical Cell ◽  
A Cell ◽  
New Type ◽  
Physiological Problem ◽  
Chemical Problem

Texperiments are described which indicate that there is a physiological problem quite apartfrom the chemical problem of luminescence in the secretion of Malacocephalus Icevis(Lowe). The luminiferous substances are present in granules, which behave as though each were bounded bya membrane whose permeabilities resemble those of a typical cell, but differ from a cell in that they have little or no power of recovery from adverse conditions.For optimal luminescence they require (i) a medium of a certain osmotic pressure,(ii) a certain range of alkalinity, (iii) a certain range of temperature, and (iv)abundant oxygen. Sea-water is not necessary for luminescence.If they are exposed to extremes of acidity or alkalinity, or of hypotonic or hypertonic solutions, irreversible changes rapidly set in in the membrane of the granule, whereby the power of luminescence is lost.In artificial conditions the rapid fading of the light from the initial brilliance is probably due to an increasing acidity caused by the accumulation of the products of oxidation.

scholarly journals NATURE OF THE ACTION CURRENT IN NITELLA

1943 ◽  
Vol 27 (1) ◽  
pp. 61-68 ◽  
Author(s):  
W. J. V. Osterhout
Keyword(s):  
Partial Response ◽  
Outer Surface ◽  
Base Line ◽  
Normal Amount ◽  
Action Current ◽  
Typical Response ◽  
Total Potential ◽  
Protoplasmic Surface ◽  
Outer Protoplasmic Surface

When a stimulus arrives before recovery is complete there may be no response or only a partial response. A typical response appears to involve an immediate loss of potential at the inner protoplasmic surface but not at the outer surface. As long as recovery is incomplete only a part of the total potential is located at the inner protoplasmic surface and the loss of this part of the total potential can cause only a partial response; i.e., one of smaller magnitude than the normal. Even after the action curve has returned to the base line recovery may be incomplete and the response only a partial one. The return of the action curve to the base line means a recovery of total potential but if part of this is located at the outer protoplasmic surface and if this part is not lost when stimulation occurs the response can be only a partial one. During recovery there is a shift of potential from the outer to the inner protoplasmic surface. Not until this shift is completed can recovery be called complete. The response to stimulation then becomes normal because the loss of potential reaches the normal amount. In many cases the partial responses appear to conform to the all-or-none law. In other cases this is doubtful.

scholarly journals ABNORMAL PROTOPLASMIC PATTERNS AND DEATH IN SLIGHTLY HYPERTONIC SOLUTIONS

1948 ◽  
Vol 31 (3) ◽  
pp. 291-300 ◽  
Author(s):  
W. J. V. Osterhout
Keyword(s):  
Outer Surface ◽  
Sea Water ◽  
External Solution ◽  
Mechanical Action ◽  
Characteristic Pattern ◽  
Hypertonic Solutions ◽  
Protoplasmic Surface ◽  
Made In

Some interesting properties of protoplasm are revealed when slightly hypertonic solutions of sugars or of electrolytes are applied to Nitella. The chloroplasts contract and the space between them increases and forms a characteristic pattern consisting of clear areas extending lengthwise along the cell and tapering off at both ends. The development of these areas is irreversible from the start. If the cell is returned to water after plasmolysis begins these areas continue to enlarge in much the same fashion as when no change is made in the external solution. The cell soon dies whether returned to water or left in the plasmolyzing solution. Similar results are obtained with other sugars, with NaCl, CaCl2, and sea water. Similar reactions are also brought about by strong ingoing or outgoing currents of water. This suggests that mechanical action may be chiefly responsible for the result and this idea is in harmony with other facts. It seems possible that the retraction of the protoplasm from the cellulose wall may disturb the delicate non-aqueous film which covers the outer surface of the protoplasm and thus produce injury. Such an effect might take place even without visible retraction if the injury occurred in protoplasmic projections extending into the cellulose wall. A study of this behavior may throw light on the nature of the protoplasmic surface and on the properties of protoplasmic gels as well as on the process of death. An understanding of the mechanism involved may help to explain the action of hypertonic solutions in other cases as, for example, in the artificial parthenogenesis of marine eggs.

scholarly journals THE EXPERIMENTAL PRODUCTION OF DOUBLE PEAKS IN CHARA ACTION CURVES AND THEIR RELATION TO THE MOVEMENT OF POTASSIUM

1940 ◽  
Vol 24 (1) ◽  
pp. 9-13
Author(s):  
W. J. V. Osterhout ◽  
S. E. Hill
Keyword(s):  
Outer Surface ◽  
Concentration Gradient ◽  
Experimental Production ◽  
Double Peaks ◽  
Protoplasmic Surface ◽  
Outer Protoplasmic Surface

The action curve in Chara seems to depend (as in Nitella) on the outward movement of K+ from the sap. Presumably the increase in permeability in the inner protoplasmic surface and the outward movement of K+ destroy the concentration gradient of K+ across the inner protoplasmic surface. Hence the outwardly directed P.D. disappears, causing the rise (spike) of the action curve. The outer protoplasmic surface is normally insensitive to K+. But when it is made sensitive to K+ by treatment with guanidine the outwardly moving K+ sets up a positive P.D. on reaching the outer surface and this causes the action curve to fall, producing a peak. Then the curve has 2 peaks, the second being due to the process of recovery. The action curve thus comes to resemble that of Nitella in which the outer protoplasmic surface is normally sensitive to K+.

Artificial Planning Experience by Means of a Heuristic Cell-Space Model: Simulating International Migration in the Urban Process

1995 ◽  
Vol 27 (10) ◽  
pp. 1647-1665 ◽  
Author(s):  
J Portugali ◽  
I Benenson
Keyword(s):  
Urban Policy ◽  
Initial Conditions ◽  
Point Of View ◽  
Town Planning ◽  
Space Model ◽  
Self Organized ◽  
A Cell ◽  
Policy And Planning ◽  
The City ◽  
Theory And Model

We suggest considering the city as a complex, open, and thus self-organized system, and describing it by means of a cell-space model. A central property of self-organizing systems is that they are not controllable—not by individuals, nor by economic, political, and planning institutions. The city, in this respect, is complex and untamable. Inability to recognize and accept this property is one of the reasons for the difficulties and problems of modernist town planning. The theory and model we present are built to describe the urban process as a historical one in which, given identical initial conditions, each simulation run is unique and never fully repeats itself. From the point of view of urban policy and planning, our heuristic model can guide decisionmakers by answering the following question: ‘given the initial conditions of an inflow of new immigrants (that is, from the ex-USSR), what possible urban scenarios can result, and what are their global structural properties?’.

Localization and expression of msp130, a primary mesenchyme lineage-specific cell surface protein in the sea urchin embryo

Development ◽  
1987 ◽  
Vol 101 (2) ◽  
pp. 255-265 ◽  
Author(s):  
J.A. Anstrom ◽  
J.E. Chin ◽  
D.S. Leaf ◽  
A.L. Parks ◽  
R.A. Raff
Keyword(s):  
Cell Surface ◽  
Sea Urchin ◽  
Sea Water ◽  
Surface Protein ◽  
Specific Cell ◽  
Cell Surface Protein ◽  
Sea Urchin Embryo ◽  
A Cell ◽  
Mesenchyme Cells ◽  
Primary Mesenchyme Cells

In this report, we use a monoclonal antibody (B2C2) and antibodies against a fusion protein (Leaf et al. 1987) to characterize msp130, a cell surface protein specific to the primary mesenchyme cells of the sea urchin embryo. This protein first appears on the surface of these cells upon ingression into the blastocoel. Immunoelectronmicroscopy shows that msp130 is present in the trans side of the Golgi apparatus and on the extracellular surface of primary mesenchyme cells. Four precursor proteins to msp130 are identified and we show that B2C2 recognizes only the mature form of msp130. We demonstrate that msp130 contains N-linked carbohydrate groups and that the B2C2 epitope is sensitive to endoglycosidase F digestion. Evidence that msp130 is apparently a sulphated glycoprotein is presented. The recognition of the B2C2 epitope of msp130 is disrupted when embryos are cultured in sulphate-free sea water. In addition, two-dimensional immunoblots show that msp130 is an acidic protein that becomes substantially less acidic in the absence of sulphate. We also show that two other independently derived monoclonal antibodies, IG8 (McClay et al. 1983; McClay, Matranga & Wessel, 1985) and 1223 (Carson et al. 1985), recognize msp130, and suggest this protein to be a major cell surface antigen of primary mesenchyme cells.

1. On the Molecular Theory of Organization

1862 ◽  
Vol 4 ◽  
pp. 436-446
Author(s):  
Bennett
Keyword(s):  
Organic Molecules ◽  
Molecular Theory ◽  
Directed Attention ◽  
Vital Force ◽  
Theory Of Organization ◽  
A Cell ◽  
The Law ◽  
Real Action

Parodying the celebrated expression of Harvey, viz., Omne animal ex ovo, it has been attempted to formularise the law of development by the expression omnis cellula e cellula, and to maintain “that we must not transfer the seat of real action to any point beyond the cell.” In the attempts which have been made to support this exclusive doctrine, and to give all the tissues and all vital properties a cell origin, the great importance of the molecular element, it seemed to the author, had been strangely overlooked. It becomes important, therefore, to show that real action, both physical and vital, may be seated in minute particles, or molecules much smaller than cells, and that we must obtain a knowledge of such action in these molecules if we desire to comprehend the laws of organization. To this end the author directed attention: 1st, To a description of the nature and mode of origin of organic molecules; 2d To a demonstration of the fact that these molecules possess inherent powers or forces, and are present in all those tissues which manifest vital force; and 3d, To a law which governs the combination, arrangement, and behaviour of these molecules during the development of organised tissue.

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